Title of Invention	DEHYDROXYFLUORINATION AGENT
Abstract	There is provided a novel, useful dehydroxyfluorination agent containing sulfuryl fluoride (SO2F2) and an organic base that is free from a free hydroxyl group in the molecule. According to the present dehydroxyfluorination agent, it is not necessary to use perfluoroalkanesulfonyl fluoride, which is not preferable in large-scale use, and it is possible to advantageously produce optically-active fluoro derivatives, which are important intermediates of medicines, agricultural chemicals and optical materials, for example, 4-fluoroproline derivatives, 2'-deoxy-2'-fluorouridine derivatives, optically-active α-fluorocarboxylate derivatives, and monofluoromethyl derivatives, even in large scale.

Title of Invention

DEHYDROXYFLUORINATION AGENT

Abstract

There is provided a novel, useful dehydroxyfluorination agent containing sulfuryl fluoride (SO2F2) and an organic base that is free from a free hydroxyl group in the molecule. According to the present dehydroxyfluorination agent, it is not necessary to use perfluoroalkanesulfonyl fluoride, which is not preferable in large-scale use, and it is possible to advantageously produce optically-active fluoro derivatives, which are important intermediates of medicines, agricultural chemicals and optical materials, for example, 4-fluoroproline derivatives, 2'-deoxy-2'-fluorouridine derivatives, optically-active α-fluorocarboxylate derivatives, and monofluoromethyl derivatives, even in large scale.

Full Text	TECHNICAL FIELD [0001] The present invention relates to a novel dehydroxyfluorination agent. BACKGROUND OF THE INVENTION [0002] "Dehydroxyfluorination reaction" for replacing hydroxyl group of a hydroxyl group-containing compound with fluorine atom is an important reaction in syntheses of fluorine-containing organic compounds. The following are typical examples. [0003] 1) a process (Patent Publication 1 and Patent Publication 2) in which a substrate having a hydroxyl group is reacted with a perfluoroalkanesulfonyl fluoride, such as perfluorobutanesulfonyl fluoride, in the presence of a special, strongly basic, organic base, such as DBU (1,8-diazabicyclo[5.4.0]undec-7-ene). [0004] 2) a process (Non-patent Publication 1) in which a substrate having a hydroxyl group is reacted with perfluorobutanesulfonyl fluoride in the presence of an organic base, such as triethylamine, and "a salt or complex comprising an organic base and hydrogen fluoride" such as triethylamine tris(hydrogen fluoride) complex. [0005] 3) a process (Patent Publications 3-6) for producing a fluoro derivative by reacting a specific hydroxy derivative with trifluoromethanesulfonyl fluoride in the presence of an organic base or in the presence of an organic base and "a salt or complex comprising an organic base and hydrogen fluoride" (such as triethylamine trisGrydrogen fluoride) complex). [0006] 4) a process (Non-patent Publication 2) in which a hydroxyl group is converted into a fluorosulfate, followed by replacement with a fluorine anion. Patent Publication 1: US Patent 5760255 specification Patent Publication 2- US Patent 6248889 specification Patent Publication 3: International Publication 2004/089968 Pamphlet (Japanese Patent Application Publication 2004-323518) Patent Publication 4- Japanese Patent Application Publication 2006-083163 Patent Publication 5: Japanese Patent Application Publication 2005-336151 Patent Publication 6: Japanese Patent Application Publication 2006008534 Non-patent Publication 1: Organic Letters (US), 2004, Vol. 6, No. 9, p. 14651468 Non-patent Publication 2: Tetrahedron Letters (UK), 1996, Vol. 37, No. 1, p. 17-20 SUMMARY OF THE INVENTION [0007] In the processes of Patent Publication 1 and Patent Publication 2, it was necessary to use a long-chain perfluoroalkanesulfonyl fluoride, which is not preferable in large-scale use, and a high-price, special organic base. In the dehydroxyfluorination reaction using a perfluoroalkanesulfonyl fluoride, a perfluoroalkanesulfonic acid is stoichiometrically produced as a by-product in the form of a salt of an organic base. Therefore, waste treatment of the acid was a large problem in conducing the reaction in large scale. In particular, long-chain perfluoroalkanesulfonic acid derivatives having a carbon number of 4 or greater are pointed out to have long-term persistence in environment and toxicity, and therefore their large-scale use is limited (for example, see FARUMASHIA Vol. 40, No. 2, 2004 with respect to perfluorooctanesulfonic acid derivatives). [0008] Also in the process of Non-patent Publication 1, there was a similar problem of using long-chain perfluorobutanesulfonyl fluoride. [0009] On the other hand, the processes of Patent Publications 3-6 are superior processes that are capable of avoiding problems of long-term persistence in environment and toxicity, since they use trifluoromethanesulfonyl fluoride having a carbon number of 1. The industrial production amount of trifluoromethanesulfonyl fluoride is, however, limited, as compared with perfluorobutanesulfonyl fluoride and perfluorooctanesulfonyl fluoride. Therefore, its obtainment in large amount was not necessarily easy. [0010] The process of Non-patent Publication 2 was not a direct fluorination reaction (see Scheme 1), due to its necessity of going through imidazole sulfate in order to convert the hydroxy derivative to the fluorosulfate. [Chemical Formula 1] Scheme 1 [0011] According to Non-patent Publication 1, it is disclosed therein that, when the dehydroxyfluorination agent comprising trifluoromethanesulfonic anhydride, triethylamine tris(hydrogen fluoride) complex and triethylamine is used, gaseous trifluoromethanesulfonyl fluoride (boiling point: -21°C) is formed in the reaction system, thereby not achieving an efficient trifluoromethanesulfonylation of a hydroxyl group of the substrate, and that a combination with high-boiling-point (64°C) perfluorobutanesulfonyl fluoride (perfluorobutanesulfonyl fluoride, triethylamine tris(hydrogen fluoride) complex and triethylamine) is preferable. This description clearly indicates that low-boiling-point trifluoromethanesulfonyl fluoride is not preferable as a perfluoroalkanesulfonyl fluoride of the dehydroxyfluorination agent. Sulfuryl fluoride used in the present invention has a further lower boiling point (-49.7°C). Thus, it has been totally unclear whether or not that can preferably be used as the dehydroxyfluorination agent. [0012] As mentioned hereinbefore, there has been a strong demand for a novel dehydroxyfluorination means that is easy in large-scale operation, for producing fluoro derivatives. [0013] From the above viewpoint, the present inventors have conducted an eager examination to find a novel dehydroxyfluorination means that is easy in large-scale operation. As a result, we have found a novel dehydroxyfluorination agent comprising sulfuryl fluoride (SO2F2) and an organic base that is free from a free hydroxyl group in the molecule, thereby reaching the present invention. [0014] Sulfuryl fluoride (SO2F2) is a compound that is widely used as a fumigant. There has been, however, no report of using the compound as a dehydroxyfluorination agent. [0015] By conducting a dehydroxyfluorination using a dehydroxyfluorination agent of the present invention, it is possible to continuously conduct a fluorosulfonylation and a fluorine substitution in one reaction vessel without isolating a fluorosulfate that is a reaction intermediate. As shown in Scheme 2, the characteristic of the present invention is that a hydroxy derivative can be converted into a fluorosulfate by using sulfuryl fluoride and that "a salt or complex comprising an organic base and hydrogen fluoride", which has been stoichiometrically produced as a by-product in the reaction system in the step of this fluorosulfonylation, can be effectively used as a fluorine source of the fluorine substitution. [0016] Furthermore, as shown in Scheme 3, in the case of using "the above dehydroxyfluorination agent further comprising a hydrogen fluoride source (it refers to hydrogen fluoride or a salt or complex formed between hydrogen fluoride and an organic salt) added from the outside of the system", as compared with the process shown in Scheme 2, it was also found that the fluoro derivative can be obtained with high yield and selectivity. [Chemical Formula 2] [0017] In the present invention, sulfuryl fluoride has two reaction points to the hydroxyl group. However, in the case of using 4-hydroxyproline derivatives, which are particularly optically active hydroxy derivatives, 1-β-D-arabinofuranosyluracil derivatives, optically active α-hydroxycarboxylate derivatives, and primary alcohol derivatives as hydroxy derivatives, it was found that a disubstituted sulfate is almost not given (see Scheme 4) and that the fluorine substitution proceeds well by going through the target fluorosulfate. We have clarified that such problem does not occur by perfluoroalkanesulfonyl fluoride and that sulfuryl fluoride can preferably be used as a dehydroxyfluorination agent. [Chemical Formula 4] [0018] Furthermore, the present inventors have found that stereochemistry of a fluoro derivative obtained by the reaction with sulfuryl fluoride is inverted, in the case of using as the hydroxyl derivative an optically active compound caused by chirality of the carbon atom that is covalently bonded with the hydroxyl group. In the present dehydroxyfluorination reaction, it is considered that the fluorosulfonylation proceeds with maintenance of stereochemistry and the subsequent fluorine substitution proceeds with inversion of stereochemistry. A dehydroxyfluorination reaction accompanied with such inversion of stereochemistry is also already disclosed in a process using a perfluoroalkanesulfonyl fluoride of Patent Publication 2. However, fluorosulfuric acid group is vastly inferior to perfluoroalkanesulfonic acid group in leaving ability [Synthesis (Germany) 1982, Vol. 2, p. 85-126]. Therefore, it was unclear whether or not the reaction proceeds with high asymmetry transcription percentage in a dehydroxyfluorination reaction, using sulfuryl fluoride, of a chain substrate, which is difficult in control of stereochemistry, particularly an optically active orhydroxycarboxylate derivative. In contrast with this, the present inventors have found that a dehydroxyfluorination using sulfuryl fluoride of the present invention proceeds well under a very mild reaction condition and that an optically active α-fluorocarboxylate derivative, which is extremely high in optical purity, is obtained by the reflection of optical purity of the optically active orhydroxycarboxylate derivative, which is used as the raw material substrate. [0019] Furthermore, it was unclear whether or not fluorosulfates that are obtained by conversion of 4-hydroxyproline derivative and 1-β-D-arabinofuranosyluracil derivative through fluorosulfonylation and that correspond to the respective raw material substrates have sufficient leaving abilities. In contrast with this too, the present inventors have found that a dehydroxyfluorination reaction using sulfuryl fluoride of the present invention can preferably be used as the process for producing 4-fluoroproline derivative and 2'deoxy2'-fluorouridine derivative. DETAILED DESCRIPTION [0020] Advantageous points of the dehydroxyfluorination agent of the present invention are described in the following, as compared with prior art. [0021] Relative to the processes of Patent Publication 1, Patent Publication 2 and Non-patent Publication 1, it is not necessary to use perfluoroalkanesulfonyl fluorides that are problematic in waste treatment, long-term persistence in environment and toxicity, and it is possible in the present invention to use sulfuryl fluoride, which is widely used as a fumigant. [0022] In the case of conducting a dehydroxyfluorination reaction using a dehydroxyfluorination agent of the present invention, fluorosulfuric acid is stoichiometrically produced as a salt of an organic base. It is, however, possible to easily treat the acid into fluorite (CaF2) as a final waste. It is thus extremely preferable for a fluorination reaction in large scale. [0023] Furthermore, the perfluoroalkyl moiety of perfluoroalkanesulfonyl fluoride is at last not incorporated into the target product. One having a less fluorine content is advantageous in atomic economy, as long as it has sufficient sulfonylation ability and leaving ability. From such a viewpoint too, sulfuryl fluoride is vastly superior. [0024] In a dehydroxyfluorination agent of the present invention, it is not necessary to use a high-price, special organic base such as DBU, and it is possible to use a low-price organic base, such as triethylamine, that is common in large-scale production. [0025] Relative to the process of Non-patent Publication 2, it is not necessary to go through imidazole sulfate. In the present invention, it is possible to directly convert a hydroxy derivative to a fluorosulfate by using sulfuryl fluoride. [0026] Furthermore, a new advantageous effect of the invention has been found by using sulfuryl fluoride. In a dehydroxyfluorination reaction using a perfluoroalkanesulfonyl fluoride, a salt of a perfluoroalkanesulfonic acid and an organic base is stoichiometrically contained in the reaction-terminated liquid. The salt, particularly a salt derived from a perfluoroalkanesulfonic acid having a carbon number of 4 or greater, has an extremely high solubility in organic solvent. We thus have found that there is a problem that it is not possible to effectively remove the salt and thereby it imposes a burden on the purification operation, even if conducting a post-treatment operation that is generally used in organic syntheses, such as washing of organic layer with water or alkali aqueous solution. Furthermore, a salt of perfluoroalkanesulfonic acid and organic base may act as an acid catalyst in some cases. Thus, it was necessary to efficiently remove the salt in order to produce a compound having an acid-labile functional group. Actually, if a large amount of a salt of perfluorobutanesulfonic acid and organic base is contained in a distillation purification of a crude product of 4-fluoroproline derivative, in which the protecting group of the secondary amino group is a tert-butoxycarbonyl (Boc) group, debutoxycarbonylation reaction is found considerably. Thus, it was not possible to recover the target product with good yield. On the other hand, a salt of fluorosulfuric acid and organic base, which is produced as a by-product in the present invention, is extremely high in solubility in water. Therefore, it can perfectly be removed by washing the organic layer with water or alkali aqueous solution. Since it does almost not impose a burden on the purification operation, it was found to be extremely preferable for a fluorination reaction in large scale. [0027] A dehydroxyfluorination agent having characteristics disclosed in the present invention has not been disclosed at all in related technical fields. It is extremely useful as a dehydroxyfluorination agent in large scale, since it is very high in selectivity and does almost not produce as by-products impurities that are difficult in separation. In particular, it can extremely preferably be used for a large-scale production process of optically active fluoro derivatives, which are important intermediates of medicines, agricultural chemicals and optical materials, specifically 4-fluoroproline derivatives, 2'-deoxy-2'-fluorouridine derivatives and optically active α-fiuorocarboxylate derivatives, and monofluoromethyl derivatives. It is capable of remarkably efficiently producing them, as compared with conventional production processes. [0028] In the following, a dehydroxyfluorination agent of the present invention is described in more detail. [0029] It is possible to prepare a dehydroxyfluorination agent of the present invention by introducing sulfuryl fluoride into a container in which an organic base exists. In order to further improve reactivity, it is also possible to further add a hydrogen fluoride source (it refers to hydrogen fluoride or a salt or complex formed between hydrogen fluoride and an organic base) from the outside of the system. Furthermore, it is also possible to add an aprotic organic solvent in order to make the reaction proceed more smoothly. [0030] Herein, the container is desirably a pressure-proof airtight container, since sulfuryl fluoride is in gas under ordinary temperature and ordinary pressure. [0031] The order of adding the reagents and the preparation method are not particularly limited, (i) It is possible to prepare a dehydroxyfluorination agent of the present invention by previously placing an organic base that is free from a free hydroxyl group in the molecule (and, according to need, "a hydrogen fluoride source added from the outside of the system" and an aprotic organic solvent) in a container, then sealing it, and introducing gaseous sulfuryl fluoride thereinto, (ii) It is also possible to previously place each component of the above, except sulfuryl fluoride, and the reaction raw material (the hydroxy derivative) into a container and successively or continuously introduce sulfuryl fluoride thereinto. In the case of (ii), the dehydroxyfluorination reaction starts at the same time when the dehydroxyfluorination agent is prepared. Like (ii), to prepare a dehydroxyfluorination agent of the present invention in the reaction system (in situ) is simpler and easier in handling. On the other hand, in large-scale production, it is practical in some cases to introduce sulfuryl fluoride in liquid state under pressurized condition. [0032] The organic base used for a dehydroxyfluorination agent of the present invention is an organic base that is free from a free hydroxyl group in the molecule. In case that a free hydroxyl group exists in a part of the base molecule, it can preferably be used by protecting those hydroxyl groups with various protecting groups. However, as compared with the use by protecting such base, it is economically more preferable to directly use one that is generally available as an organic base with low price. In particular, a base is preferable that is selected from the group consisting of trimethylamine, triethylamine, diisopropylethylamine, tri-n-propylamine, pyridine, 2,3-lutidine, 2,4-lutidine, 2,5-lutidine, 2,6-lutidine, 3,4-lutidine, 3,5'lutidine, 2,3,4-collidine, 2,4,5-collidine, 2,5,6'collidine, 2,4,6-collidine, 3,4,5-collidine, 3,5,6-collidine, and the like. Particularly, triethylamine, diisopropylethylamine, pyridine, 2,4-lutidine, 2,6-lutidine, 3,5-lutidine, and 2,4,6-collidine are preferable. [0033] The present inventors have found that reactivity of the dehydroxyfluorination improves strikingly by further adding "hydrogen fluoride source" to the dehydroxyfluorination agent of the present invention. Herein, "hydrogen fluoride source" refers to hydrogen fluoride or a salt or complex formed between hydrogen fluoride and an organic base. [0034] As shown in Scheme 2, in the dehydroxyfluorination reaction of the present invention, firstly in the fluorosulfate formation, an equimolar amount of hydrogen fluoride (this hydrogen fluoride may form a salt or complex with the organic base) is generated in the system. This hydrogen fluoride becomes a fluorine source in the subsequent fluorine substitution, and it conducts a nucleophilic attack against the fluorosulfate of the reaction intermediate. With this, the fluorine substitution proceeds. This fluorine substitution is markedly accelerated when hydrogen fluoride is in an excessive condition by the addition of the hydrogen fluoride source from the outside of the system. In particular, it was found that a great effect is generated in the case of dehydroxyfluorinating a hydroxy derivative that is low in reactivity. [0035] In a dehydroxyfluorination agent of the present invention, the ratio of sulfuryl fluoride by mol number to the organic base is not particularly limited. However, as shown in Scheme 2, the ratio of sulfuryl fluoride, which is consumed in the dehydroxyfluorination reaction, by mol number to the organic base is 1:1 in theory. Therefore, in principle, it suffices that the ratio of both is about 1:1. However, it is possible in some cases to obtain a higher reactivity by excessively using one of both. Specifically, the ratio of sulfuryl fluoride by mol number to the organic base is preferably in a range of roughly 5:1-1:5. [0036] Furthermore, in the dehydroxyfluorination agent of the present invention, in the case of adding "hydrogen fluoride or a salt or complex formed between hydrogen fluoride and an organic base (e.g., triethylamine tris(hydrogen fluoride) complex)" as a hydrogen fluoride source from the outside of the system, the ratio of sulfuryl fluoride by mol number to the above hydrogen fluoride source (in terms of HF) is preferably in a range of roughly 3:1-1:10, more preferably in a range of 1:1-1:10. If the mol number (in terms of HF) of the hydrogen fluoride source is less than 1/3 of the mol number of sulfuryl fluoride, the effect of positively adding it is low. If it is greater than 10 times that, it becomes disadvantageous in economy and production. [0037] As these organic bases used for "the salt or complex comprising an organic base and hydrogen fluoride" added from the outside of the system, it is possible to preferably use any of the types mentioned as "the organic base that is free from a free hydroxyl group in the molecule", which is an essential element of the present invention. This organic base in the salt or complex may be of a type that is different from the organic base that is an essential element of the present invention, but being the same type is simple. Still triethylamine is one of particularly preferable ones. [0038] In the case of using a salt or complex comprising an organic base and hydrogen fluoride, the molar ratio of the organic base to the hydrogen fluoride in this salt or complex is in a range of 100:1-1:100, preferably in a range of 50:1-1:50 in general, more preferably in a range of 25:1-1:25 in particular. Furthermore, it is extremely convenient to use "a complex comprising 1 mol of triethylamine and 3 mols of hydrogen fluoride" and "a complex comprising ~30% (-10 mol%) of pyridine and -70% (~90mol%) of hydrogen fluoride", which are placed on sale from Aldrich (Aldrich, 2003-2004 Comprehensive Catalogue). [0039] Apart from the above-mentioned organic base, it is desirable to further add an aprotic organic solvent in order to have a mutual affinity between sulfuryl fluoride and the organic base in a dehydroxyfluorination agent of the present invention. As such aprotic organic solvent, it is possible to mention aliphatic hydrocarbon series such as n-hexane, cyclohexane and n-heptane; aromatic hydrocarbon series such as benzene, toluene, xylene and mesitylene; halogenated hydrocarbon series such as methylene chloride, chloroform and 1,2'dichloroethane; ether series such as diethyl ether, tetrahydrofuran and tert-butyl methyl ether; ester series such as ethyl acetate and n-butyl acetate; amide series such as N,N-dimethylformamide, N,N-dimethylacetamide and N-methylpyrrolidone; nitrile series such as acetonitrile and propionitrile; dimethylsulfoxide,' and the like. Of these, n-heptane, toluene, mesitylene, methylene chloride, tetrahydrofuran, ethyl acetate, N,N-dimethylformamide, N,N-dimethylacetamide, acetonitrile, propionitrile, and dimethylsulfoxide are preferable. In particular, toluene, mesitylene, methylene chloride, tetrahydrofuran, N,N-diemethylformamide, and acetonitrile are more preferable. It is possible to use these reaction solvents alone or in combination. [0040] The amount of the aprotic organic solvent is not particularly limited. It suffices to use 0.1L (liter) or greater, preferably 0.1-20L in general, more preferably 0.1-10L in particular, relative to 1 mole of sulfuryl fluoride. [0041] By using a dehydroxyfluorination agent of the present invention, it is possible to continuously conduct the fluorosulfonylation and the fluorine substitution in one reactor without separation of the fluorosulfate, which is a reaction intermediate. [0042] Furthermore, in the fluorosulfonylation, stereochemistry of the hydroxyl group is maintained, and stereochemistry is inverted in the subsequent fluorine substitution. Therefore, 4-fluoroproline derivative in 4S/2R configuration is obtained from 4-hydroxyproline derivative in 4R/2R configuration. Similarly, 4R/2R configuration from 4S/2R configuration, 4S/2S configuration from 4R/2S configuration, and 4R/2S configuration from 4S/2S configuration. Optically active crfluorocarboxylate derivative in S configuration at α-position is obtained from optically active α-hydroxycarboxylate derivative in R configuration at α-position. Similarly, R configuration at crposition is obtained from S configuration at a-position with good selectivity. [0043] [Regarding Hydroxy Derivative] According to a dehydroxyfluorination agent of the present invention, it is possible to substitute F atom for OH group of various hydroxy derivatives (they refer to compounds having at least one free hydroxyl group in the molecule). In the following, a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, is described. [0044] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite a hydroxy derivative represented by the general formula [1], [Chemical Formula 5] [in the formula, each of R, R1 and R2 independently represents a hydrogen atom, alkyl group, substituted alkyl group, aromatic ring group, or alkoxycarbonyl group]. By dehydroxyfluorinating the present compound, it is possible to obtain a fluoro derivative represented by the general formula [2], [Chemical Formula 6] [in the formula, R, R1 and R2 are defined as in the general formula [1]]. [0045] When R, R1 and R2 of the hydroxyl derivative represented by the general formula [1] are alkyl groups, substituted alkyl groups, aromatic ring groups or alkoxycarbonyl groups other than hydrogen atoms, they also can have an optically active moiety caused by chirality of carbon atom, axis and the like. In these cases, stereochemistry of the optically active moiety is maintained through the fluorination reaction of the present invention. [0046] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite a hydroxy derivative represented by the general formula [la], [Chemical Formula 7] [In the formula, each of R, R1 and R2 independently represents a hydrogen atom, alkyl group, substituted alkyl group, aromatic ring group, or alkoxycarbonyl group. The alkyl group is defined as being a C1C16 straight-chain or branched alkyl group. The substituted alkyl group is defined as being an alkyl group, in which a halogen atom, lower alkoxy group, lower haloalkoxy group, lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group (CONH2), unsaturated group, aromatic ring group, nucleic acid base, aromatic-ring oxy group, aliphatic heterocyclic group, protected hydroxyl group, protected amino group, protected thiol group, or protected carboxyl group has been substituted therefor by any number and by any combination on any carbon atom of the alkyl group. Any carbon atoms themselves of any two alkyl groups or substituted alkyl groups may form a covalent bond to have an aliphatic ring, and carbon atoms of the aliphatic ring may be partially replaced with nitrogen atom or oxygen atom to have an aliphatic heterocyclic ring. The aromatic ring group is defined as being an aromatic hydrocarbon group or aromatic heterocyclic group containing oxygen atom, nitrogen atom or sulfur atom. The alkoxycarbonyl group is defined as being an alkoxycarbonyl group comprising an C1-C12 straight-chain or branched alkoxy group, and any carbon atoms themselves of the alkoxy group and of any alkyl group or substituted alkyl group may form a covalent bond to have a lactone ring.]. By dehydroxyfluorinating the present compound, it is possible to obtain a fluoro derivative represented by the general formula [2a], [Chemical Formula 8] [in the formula, R, R1 and R2 are defined as in the general formula [la]]. [0047] The substituted alkyl group of R, R1 and R2 of the hydroxy derivative represented by the general formula [la] is defined as being "an alkyl group, in which a halogen atom of fluorine, chlorine, bromine and iodine; lower alkoxy group such as methoxy group, ethoxy group and propoxy group; lower haloalkoxy group such as fluoromethoxy group, chloromethoxy group and bromomethoxy group; lower alkylamino group such as dimethylamino group, diethylamino group and dipropylamino group,' lower alkylthio group such as methylthio group, ethylthio group and propylthio group; cyano group; aminocarbonyl group (CONH2); unsaturated group such as alkenyl group and alkynyl group; aromatic ring group such as phenyl group and naphthyl group; nucleic acid base such as adenine residue, guanine residue, hypoxanthine residue, xanthine residue, uracil residue, thymine residue and cytosine residue; aromaticring oxy group such as phenoxy group and naphthoxy group,' aliphatic heterocyclic group such as piperidyl group, piperidino group and morpholyl group; protected hydroxyl group, protected amino group, protected thiol group, protected carboxyl group, or the like has been substituted therefor by any number and by any combination on any carbon atom of the alkyl group". [0048] In the present specification, each of the following terms is used as having the following meaning. "Lower" means C1-C6 straight-chain or branched. In case that "unsaturated group" is a double bond, it can be in a geometrical isomerism of either E configuration or Z configuration. "Aromatic ring group" also can be an aromatic heterocyclic group (containing a condensed skeleton) containing oxygen atom, nitrogen atom, sulfur atom and the like, such as furyl group, pyrrolyl group and thienyl group, other than aromatic hydrocarbon groups. "Nucleic acid base" can be protected with a protecting group that is generally used in the field of syntheses of nucleic acid related substances (For example, as a protecting group of hydroxyl group, it is possible to mention acyl groups such as acetyl group and benzoyl group; alkyl groups such as methoxymethyl group and allyl group; and aralkyl groups such as benzyl group and triphenylmethyl group. As a protecting group of amino group, it is possible to mention acyl groups such as acetyl group and benzoyl group and aralkyl groups such as benzyl group. Furthermore, halogen atom, lower alkyl group, lower alkoxy group and the like can be substituted in these protecting groups.). Furthermore, hydrogen atom, hydroxyl group and amino group of "nucleic acid base" can be replaced with hydrogen atom, amino group, halogen atom, lower alkyl group, lower alkenyl group nitro group and the like. As "protecting groups of hydroxyl group, amino group, thiol group and carboxyl group", it is possible to use protecting groups and the like described in Protective Groups in Organic Synthesis, Third Edition, 1999, John Wiley & Songs, Inc. In "unsaturated group", "aromatic ring group", "aromatic ring oxy group" and "aliphatic heterocyclic group", it is possible to substitute lower alkyl group, halogen atom, lower haloalkyl group, lower alkoxy group, lower haloalkoxy group, lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group, protected hydroxyl group, protected amino group, protected thiol group, protected carboxyl group, and the like. [0049] Alkyl group and substituted alkyl group of R, R1 and R2 of the hydroxy derivative represented by the general formula [la] also can be an aliphatic ring, such as cyclopentane ring and cyclohexane ring, by the formation of a covalent bond by any carbon atoms of any two alkyl groups or substituted alkyl groups. They also can be an aliphatic heterocyclic ring, such as pyrrolidine ring (also containing a protected secondary amino group), piperidine ring (also containing a protected secondary amino group), oxolane ring and oxane ring, in which carbon atoms of the aliphatic ring have been partially replaced with nitrogen atoms or oxygen atoms. [0050] Aromatic ring group of R, R1 and R2 of the hydroxy derivative represented by the general formula [la] is defined as being "an aromatic hydrocarbon group, such as phenyl group, naphthyl group and anthryl group, or aromatic heterocyclic group containing oxygen atom, nitrogen atom, sulfur atom or the like, such as furyl group, pyrrolyl group, thienyl group, benzofuryl group, indolyl and benzothienyl group. In these aromatic hydrocarbon groups and aromatic heterocyclic groups, it also possible to substitute lower alkyl group, halogen atom, lower haloalkyl group, lower alkoxy group, lower haloalkoxy group, lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group, unsaturated group, aromatic ring group, aromatic ring oxy group, aliphatic heterocyclic group, protected hydroxyl group, protected amino group, protected thiol group, protected carboxyl group, and the like. [0051] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite an optically active hydroxy derivative represented by the general formula [3], [Chemical Formula 9] [In the formula, each of R and R1 is independently an alkyl group, substituted alkyl group, or alkoxycarbonyl group. * represents an asymmetric carbon (R and R' do not take the same substituent). The alkyl group is defined as being a C1-C16 straight-chain or branched alkyl group. The substituted alkyl group is defined as being an alkyl group, in which a halogen atom, lower alkoxy group, lower haloalkoxy group, lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group (CONH2), unsaturated group, aromatic ring group, nucleic acid base, aromatic-ring oxy group, aliphatic heterocyclic group, protected hydroxyl group, protected amino group, protected thiol group, or protected carboxyl group has been substituted therefor by any number and by any combination on any carbon atom of the alkyl group. Any carbon atoms themselves of two alkyl groups or substituted alkyl groups may form a covalent bond to have an aliphatic ring, and carbon atoms of the aliphatic ring may be partially replaced with nitrogen atom or oxygen atom to have an aliphatic heterocyclic ring. The alkoxycarbonyl group is defined as being an alkoxycarbonyl group comprising an C1-C12 straight-chain or branched alkoxy group, and any carbon atoms themselves of the alkoxy group and of any alkyl group or substituted alkyl group may form a covalent bond to have a lactone ring. Stereochemistry of the carbon atom, to which the hydroxyl group is covalently bonded, is inverted through the reaction.] By dehydroxyfluorinating the present compound, it is possible to obtain an optically active fluoro derivative represented by the general formula [4], [Chemical Formula 10] [In the formula, R, R1 and * are defined as in the general formula [3]]. [0052] The dehydroxyfluorination reaction of the present invention becomes particularly effective for the production of high-optical-purity fluoro derivatives, which are required for important intermediates of medicines, agricultural chemicals and optical materials. In order to maximize this effect, the selection of the raw material substrate is important. Specifically, although it can be applied to optically active tertiary alcohol derivatives, which are sterically bulky, optically active secondary alcohol derivatives (corresponding to optically active hydroxy derivatives represented by the general formula [3]), which can be expected to have a high asymmetry transcription percentage, are still more preferable. Furthermore, the substituents of the optically active secondary alcohol derivative (corresponding to R and R' of the optically active hydroxy derivative represented by the general formula [3]) are preferably alkyl group, substituted alkyl group and alkoxycarbonyl group, as compared with aromatic ring groups, which are expected to be accompanied with a partial racemization by going through a transition state, such as the benzyl-position carbonium ion, in the course of the fluorine substitution of the fluorosulfate as the reaction intermediate. [0053] Due to the usefulness of the product to be obtained, the carbon number of the alkyl group is generally preferably 1 to 14, particularly more preferably 1 to 12. The substituents of the substituted alkyl group are preferably nucleic acid base, protected hydroxyl group, protected amino group, and protected carboxyl group. It is preferable that two alkyl groups or substituted alkyl groups take an aliphatic heterocyclic ring. The carbon number of the alkoxy group of the alkoxycarbonyl group is generally preferably 1 to 10, particularly more preferably 1 to 8. [0054] Furthermore, stereochemistry of the asymmetric carbon of the optically active secondary alcohol derivative (corresponding to the optically active hydroxy derivative represented by the general formula [3]) can be R configuration or S configuration. Enantiomer excess ratio (%ee) is not particularly limited. It suffices to use one having 90%ee or greater. In general, 95%ee or greater is preferable, and particularly 97%ee is more preferable. [0055] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite a 4-hydroxyproline derivative represented by the general formula [5], [Chemical Formula 11] [In the formula, R3 represents a protecting group of the secondary amino group, R4 represents a protecting group of the carboxyl group, * represents an asymmetric carbon, and stereochemistry of the 4-position is inverted through the reaction, and stereochemistry of the 2-position is maintained.] By dehydroxyfluorinating the present compound, it is possible to obtain a 4-fluoroproline derivative represented by the general formula [6], [Chemical Formula 12] [In the formula, R3, R4 and * are defined as in the general formula [5]]. [0056] As the protecting group R3 of the secondary amino group of the 4-hydroxyproline derivative represented by the general formula [5], it is possible to mention benzyloxycarbonyl (Z) group, tert-butoxycarbonyl (Boc) group, 9-fluorenylmethoxycarbonyl (Fmoc) group, 3-nitro-2-pyridinesulfenyl (Npys) group, p-methoxybenzyloxycarbonyl [Z(MeO)] group, and the like. Of these, benzyloxycarbonyl (Z) group and tert-butoxycarbonyl (Boc) group are preferable, and particularly tert-butoxycarbonyl (Boc) group is more preferable. [0057] As the protecting group R4 of the carboxyl group of the 4-hydroxyproline derivative represented by the general formula [5], it is possible to mention methyl (Me) group, ethyl (Et) group, tert-butyl (t-Bu) group, trichloroethyl (Tce) group, phenacyl (Pac) group, benzyl (Bzl) group, 4-nitrobenzyl [Bzl(4"NO2)] group, 4-methoxybenzyl [Bzl(4"MeO)] group, and the like. Of these, methyl (Me) group, ethyl (Et) group and benzyl (Bzl) group are preferable, and particularly methyl (Me) group and ethyl (Et) group are more preferable. [0058] It is possible to produce the 4-hydroxyproline derivative represented by the general formula [5] from a commercial optically active 4-hydroxyproline by referring to 4th Edition Jikken Kagaku Koza 22 Organic Synthesis IV Acid, Amino acid, Peptide (Maruzen, 1992, p. 193-309). Depending on a combination of the protecting group R3 of the secondary amino group and the protecting group R4 of the carboxyl group, there are commercial products, and it is also possible to use these. Of the 4-hydroxyproline derivative represented by the general formula [5], it is possible to easily convert a hydrochloride of optically active 4-hydroxyproline methyl ester into one in which the protecting group R3 of the secondary amino group is a tert-butoxycarbonyl (Boc) group and in which the protecting group R4 of the carboxyl group is a methyl (Me) group, in accordance with Tetrahedron Letters (United Kingdom), 1988, Vol. 39, No. 10, p. 1169-1172. [0059] As stereochemistry of the asymmetric carbon of the 4-hydroxyproline derivative represented by the general formula [5], each of 2-position and 4-position can independently take R configuration or S configuration. As a combination of stereochemistry, there is 4R/2R form, 4S/2R form, 4R/2S form or 4S/2S form. Enantiomer excess ratio (%ee) or diastereomer excess ratio (%de) of each stereoisomer is not particularly limited. It suffices to use 90%ee or 90%de or greater, normally preferably 95%ee or 95%de or greater, particularly more preferably 97%ee or 97%de or greater. [0060] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite a 1-β-D-arabinofuranosyluracil derivative represented by the general formula [7], [Chemical Formula 13] [In the formula, each of R5 and R6 independently represents a protecting group of the hydroxyl group.]. By dehydroxyfluorinating the present compound, it is possible to obtain a 2'-deoxy-2'-fluorouridine derivative represented by the general formula [8], [Chemical Formula 14] [In the formula, R5 and R6 are defined as in the general formula [7].]. [0061] As the protecting groups R5 and R6 of the hydroxyl groups of the 1-β-D-arabinofuranosyluracil derivative represented by the general formula [7], it is possible to mention trithyl group (triphenylmethyl group), tetrahydropyranil group (THP group), and tetrahydrofuranyl group (THF group). Of these, tetrahydropyranil group (THP group), and tetrahydrofuranyl group (THF group) are preferable, and particularly tetrahydropyranil group (THP group) is more preferable. It is possible to produce 1-β-D-arabinofuranosyluracil derivative represented by the general formula [7] by referring to Chem. Pharm. Bull. (Japan), 1994, Vol. 42, No. 3, p. 595-598 and Khim. Geterotsikl. Soedin. (Russia), 1996, No. 7, p. 975-977. It is possible to obtain one, in which hydroxyl groups of 3'-position and 5'-position are selectively protected, by following the processes of these publications. [0062] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite an optically-active, a-hydroxycarboxylate derivative represented by the general formula [9], [Chemical Formula 15] [In the formula, R7 represents a C1-C12 alkyl group or substituted alkyl group, R8 represents a C1-C8 alkyl group, any carbon atoms themselves of the alkyl group or of the substituted alkyl group of R7 and R8 may form a covalent bond to have a lactone ring, * represents an asymmetric carbon, and stereochemistry of the orposition is inverted through the reaction.]. By dehydroxyfluorinating the present compound, it is possible to obtain an optically-active, α-fluorocarboxylate derivative represented by the general formula [10], [Chemical Formula 16] [In the formula, R7, R8 and * are defined as in the general formula [9].]. [0063] As R7 of the optically active orhydroxycarboxylate derivative represented by the general formula [9], it is possible to mention methyl group, ethyl group, propyl group, butyl group, amyl group, hexyl group, heptyl group, octyl group, nonyl group, decyl group, undecyl group, and lauryl group. The alkyl group having a carbon number of 3 or greater can be straight-chain or branched. On any carbon atom of the alkyl group, it is possible to substitute one or any combination of two of aromatic hydrocarbon groups such as phenyl group and naphthyl group, unsaturated hydrocarbon groups such as vinyl group, C1-C6 straight-chain or branched alkoxy groups, aryloxy groups such as phenoxy group, halogen atoms (fluorine, chlorine, bromine and iodine), protected carboxyl groups, protected amino groups, or protected hydroxyl groups. As the protecting groups of the carboxyl group, amino group and hydroxyl group, similar to the above, it is possible to use protecting groups described in Protective Groups in Organic Synthesis, Third Edition, 1999, John Wiley & Sons, Inc. Specifically, it is possible to mention ester group and the like as the protecting group of the carboxyl group. It is possible to mention benzyl group, acyl groups (acetyl group, chloroacetyl group, benzoyl group, 4-methylbenzoyl group and the like), and phthaloyl group, and the like as the protecting group of the amino group. It is possible to mention benzyl group, 2-tetrapyranil group, acyl groups (acetyl group, chloroacetyl group, benzoyl group, 4-methylbenzoyl group and the like), silyl groups (trialkylsilyl group, alkylarylsilyl group and the like), and the like, as the protecting group of the hydroxyl group. In particular, it is possible to mention a protecting group or the like that forms 2,2-dimethy1-1,3-dioxolane, as the protecting group of the 1,2-dihydroxy group. [0064] Although the production process, which is the target of the present invention, can be used even in case that R7 of the optically active orhydroxycarboxylate derivative represented by the general formula [9] is an aromatic hydrocarbon group, optical purity of the target product, optically active a-fluorocarboxylate derivative (R7 = an aromatic hydrocarbon group) represented by the general formula [10], lowers significantly, as compared with a case that R7 is an alkyl group or substituted alkyl group. Therefore, an alkyl group or substituted alkyl group is preferable as R7 of the optically active orhydroxycarboxylate derivative represented by the general formula [9]. [0065] As R8 of the optically active a-hydroxycarboxylate derivative represented by the general formula [9], it is possible to mention methyl group, ethyl group, propyl group, butyl group, amyl group, hexyl group, heptyl group, and octyl group. The alkyl group having a carbon number of 3 or greater can be straight-chain or branched. [0066] Stereochemistry of the asymmetric carbon of the optically active orhydroxycarboxylate derivative represented by the general formula [9] can be R configuration or S configuration. Enantiomer excess ratio (%ee) is not particularly limited. It suffices to use one having 90%ee or greater. In general, 95%ee or greater is preferable, and particularly 97%ee is more preferable. [0067] The optically active orhydroxycarboxylate derivative represented by the general formula [9] can be produced similarly from various, commercial, optically-active, oramino acids by referring to Synthetic Communications (US), 1991, Vol. 21, No. 21, p. 2165-2170. A commercial product was used as (S)-ethyl lactate used in the Examples. [0068] As a hydroxy derivative, to which a dehydroxyfluorination agent of the present invention can be applied, it is possible to cite a primary alcohol derivative represented by the general formula [11], [Chemical Formula 17] [In the formula, R represents an alkyl group or substituted alkyl group, the alkyl group is defined as being a C1-C16 straight-chain or branched alkyl group, and the substituted alkyl group is defined as being an alkyl group, in which a halogen atom, lower alkoxy group, lower haloalkoxy group, lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group (CONH2), unsaturated group, aromatic ring group, nucleic acid base, aromatic-ring oxy group, aliphatic heterocyclic group, protected hydroxyl group, protected amino group, protected thiol group, or protected carboxyl group has been substituted therefor by any number and by any combination on any carbon atom of the alkyl group.]. By dehydroxyfluorinating the present compound, it is possible to obtain a monofluoromethyl derivative represented by the general formula [12], [Chemical Formula 18] [In the formula, R is defined as in the general formula [11].]. [0069] In the development of medicines having new effectiveness, "monofluoromethyl group" is recognized as being an important motif. Thus, primary alcohol derivatives (corresponding to the primary alcohol derivative represented by the general formula [11]), which can efficiently produce monofluoromethyl derivatives (corresponding to the monofluoromethyl derivative represented by the general formula [12]), are also preferable substrates. [0070] The optically active hydroxy derivative represented by the general formula [3], the 4-hydroxyproline derivative represented by the general formula [5], 1-β-D-arabinofuranosyluracil derivative represented by the general formula [7], the optically active orhydroxycarboxylate derivative represented by the general formula [9], and the primary alcohol derivative represented by the general formula [11] are particularly preferable as the hydroxy derivative represented by the general formula [1]. [0071] [Reaction Conditions of Dehydroxyfluorination] The amount of sulfuryl fluoride (SO2F2) used in the dehydroxyfluorination agent of the present invention relative to 1mol of the hydroxy derivative is not particularly limited. It suffices to use lmol or greater, preferably 1-10 moles in general, and more preferably 1-5 moles in particular. [0072] The amount of the organic base used in the dehydroxyfluorination of the present invention relative to lmol of the hydroxy derivative is not particularly limited. It suffices to use lmol or greater, preferably 1-20 moles in general, more preferably 1-10 moles in particular. [0073] The amount of the hydrogen fluoride source (it refers to hydrogen fluoride or a salt or complex formed between hydrogen fluoride and organic base) used in the dehydroxyfluorination agent of the present invention relative to lmol of the hydroxy derivative is not particularly limited. It suffices to use 0.3moles or greater, preferably 0.5-50 moles in general, more preferably 0.725 moles in particular. [0074] The temperature condition of the dehydroxyfluorination of the present invention is not particularly limited. It suffices to conduct it in a range of-100 to +100°C, preferably -80 to +80°C in general, more preferably -60 to +60°C in particular. In the case of conducting the reaction under a temperature condition that is not lower than boiling point (-49.7°C) of sulfuryl fluoride, it is possible to use a pressure-proof reaction vessel. [0075] The pressure condition of the dehydroxyfluorination of the present invention is not particularly limited. It suffices to conduct it in a range of atmospheric pressure to 2MPa, preferably atmospheric pressure to 1.5MPa in general, more preferably atmospheric pressure to 1MPa in particular. Therefore, it is preferable to conduct the reaction using a pressure-proof reaction vessel made of a material such as stainless steel (SUS) or glass (glass lining). [0076] The reaction time of the dehydroxyfluorination of the present invention is not particularly limited. It suffices to conduct it in a range of 0.1 to 72 hours. Since it depends on substrate and the reaction conditions, it is preferable to determine the time, at which the raw material has almost disappeared, as the end point, while tracing the progress of the reaction by an analytical means such as gas chromatography, liquid chromatography, or NMR. [0077] The post-treatrrfent of the dehydroxyfluorination of the present invention is not particularly limited. Normally, it is possible to obtain a crude product by pouring the reaction-terminated liquid into water or an aqueous solution of inorganic base (for example, sodium hydrogencarbonate, potassium hydrogencarbonate, sodium carbonate or potassium carbonate) of alkali metal, followed by extraction with an organic solvent (for example, toluene, mesitylene, methylene chloride or ethyl acetate). A salt formed of fluorosulfuric acid and organic base or an alkali metal salt of fluorosulfuric acid, which is produced as a by-product from sulfuryl fluoride, is remarkably high in distribution to water. Therefore, it is possible to efficiently remove these salts by an easy operation such as washing with water and to obtain the target fluoro derivative with high chemical purity. According to need, it can be purified to have a higher chemical purity by activated carbon treatment, distillation, recrystallization and the like. EXAMPLES [0078] In the following, embodiments of the present invention are specifically explained by examples. The present invention is, however, not limited to these examples. [0079] [EXAMPLE 1] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 2.45g (9.99mmol, 1.00eq) of 4-hydroxyproline derivative represented by the following formula, [Chemical Formula 19] as a brown-color, oil-like substance. The recovered amount of the crude product was slightly greater than the weight of the theoretical yield. 10.0mLof acetonitrile, and 1.10g (10.87mmol, 1.09eq) of triethylamine, followed by lowering the inside temperature to -40°C and then bubbling 2.00g (I9.60mmol, 1.96eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 20 hours and 20 minutes. Conversion of the reaction was found by gas chromatography measurement to be 100%. The reaction-terminated liquid was poured into a potassium carbonate aqueous solution [prepared from 2.80g (20.26mmol, 2.03eq) of potassium carbonate and 50.0mL of water], followed by extraction two times with 50.0mL of ethyl acetate. The recovered organic layer was concentrated under reduced pressure, followed by vacuum drying, thereby obtaining a crude product of 4-fluoroproline derivative represented by the following formula, [Chemical Formula 20] Selectivity of the crude product was found by gas chromatography measurement to be 82.4% (As major three kinds of impurities were named Impurities A-C, Impurity A, Impurity B and Impurity C were respectively contained by 8.2%, 3.3% and 4.9%.) Instrument data of the crude product of the obtained 4-fluoroproline derivative are shown in the following (assigned as a mixture of E/Z isomers resulting from the NBoc group). It was found by 19F-NMR spectrum that the crude product did not contain at all a salt (FSO3H Et3N or FSO3K) derived from fluorosulfuric acid. [0080] 1H-NMR (standard substance: Me4Si, heavy solvent: CDCl3), 5ppm: 1.43&1.49 (sx2, total 9H), 1.95-2.55 (total 2H), 3.51-3.94 (total 2H), 3.75 (S, 3H), 4.36-4.58 (total 1H), 5.10-5.31 (total 1H). 19F-NMR (standard substance: C6F6) heavy solvent: CDCl3), 5ppm: -11.27 (total 1F). [0081] [EXAMPLE 2] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 2.45g (9.99mmol, l.OOeq) of 4-hydroxyproline derivative represented by the following formula, [Chemical Formula 21] 13.0mL of acetonitrile, 3.50g (34.59mmol, 3.46eq) of triethylamine, and 1.60g (9.92mmol, 0.99eq) of triethylamine tris(hydrogen fluoride) complex, followed by lowering the inside temperature to -40°C and then bubbling 2.00g (l9.60mmol, 1.96eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 20 hours. Conversion of the reaction was found by gas chromatography measurement to be 100%. The reaction-terminated liquid was poured into a potassium carbonate aqueous solution [prepared from 6.30g (45.58mmol, 4.56eq) of potassium carbonate and 100.0mL of water], followed by extraction two times with 100.0mL of ethyl acetate. The recovered organic layer was concentrated under reduced pressure, followed by vacuum drying, thereby obtaining a crude product of 4-fluoroproline derivative represented by the following formula, [Chemical Formula 22] as a brown-color, oil-like substance. The recovered amount of the crude product was slightly greater than the weight of the theoretical yield. Selectivity of the crude product was found by gas chromatography measurement to be 91.0% (As major three kinds of impurities were named Impurities A-C, Impurity A, Impurity B and Impurity C were respectively contained by 6.4%, 2.4% and 0.1%.) Instrument data of the crude product of the obtained 4-fluoroproline derivative were similar to those of Example 1. [0082] [EXAMPLE 3] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 12.30g (29.82mmol, 1.00eq) of 1-β-D-arabinofuranosyluracil derivative represented by the following formula, [Chemical Formula 23] 38.0mL of acetonitrile, 18.15g (l79.37mmol, 6.02eq) of triethylamine, and 19.30g (ll9.71mmol, 4.01eq) of triethylamine tris(hydrogen fluoride) complex, followed by lowering the inside temperature to -40°C and then bubbling lO.OOg (97.98mmol, 3.29eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 16 hours and 30 minutes and then at 40°C for 5 hours and 30 minutes. Conversion of the reaction was found by liquid chromatography measurement to be not lower than 99%. The reaction-terminated liquid was poured into a potassium carbonate aqueous solution [prepared from 58.00g (419.65mmol, 14.07eq) of potassium carbonate and 300.0mL of water], followed by extraction two times with 300.0mL of ethyl acetate. The recovered organic layer was washed with 200.0mL of 10% brine, followed by concentration under reduced pressure and vacuum drying, thereby obtaining 12.83g of a crude product of 2'-deoxy-2'-fluorouridine derivative represented by the following formula, [Chemical Formula 24] as a brown-color, oil-like substance. The recovered amount of the crude product was slightly greater than the weight of the theoretical yield. Selectivity of the crude product was found by liquid chromatography measurement to be 83.2%. Instrument data of the crude product of the obtained 2'-deoxy-2'-fluorouridine derivative are shown in the following (four kinds of diastereomers resulting from two THP groups were observed). [0083] 19F-NMR (standard substance: C6F6, heavy solvent: CDC13), 5ppm: -43.13 (dt, 51.9Hz, 15.4Hz), -42.50 (dt, 51.5Hz, 15.4Hz), -37.62 (dt, 51.5Hz, 15.0Hz), -37.55 (dt, 51.9Hz, 15.0Hz)/total 1F. [0084] [EXAMPLE 4] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 9.60g (81.27mmol, l.OOeq, optical purity: 98.4%ee) of an optically-active, orhydroxyearboxylate derivative represented by the following formula, [Chemical Formula 25] Selectivity of the crude product was found by gas chromatography 27.0mL of mesitylene, and 8.50g (84.00mmol, 1.03eq) of trie thy lamine, followed by lowering the inside temperature to -40°C and then bubbling 11.50 g (ll2.68mmol, 1.39eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 22 hours and 10 minutes. Conversion of the reaction was found by gas chromatography measurement to be 100%. The reaction-terminated liquid was poured into a potassium carbonate aqueous solution [prepared from 7.90g (57.16mmol, 0.70eq) of potassium carbonate and 100.0mL of water], followed by extraction two times with 45.0mL of mesitylene. The recovered organic layer was washed with a hydrochloric acid brine (prepared from 95.0mL of 1N hydrochloric acid and 10.00g of common salt), thereby obtaining 110.63g of a mesitylene solution of a crude product of an optically-active, orfluorocarboxylate derivative represented by the following formula. [Chemical Formula 26] measurement to be not less than 99.0% (except mesitylene). The mesitylene solution of the crude product was subjected to a fractional distillation (81-90°C/20000Pa), thereby recovering 26.82g of a main fraction. The main fraction was found by 1H-NMR spectrum to contain 46.90mmol of the optically-active, orfluorocarboxylate derivative, and the main fraction concentration was 21.0wt%. The total yield was 58%. Optical purity and instrument data of the main fraction of the obtained optically-active, orfluorocarboxylate derivative are shown in the following. [0085] Optical purity: 97.7%ee (It was determined by conducting a hydride reduction using excessive aluminum lithium hydride in tetrahydrofuran, then by leading the obtained (R)-2-fluoro-l-propanol into Mosher ester, and then by conducting gas chromatography. Asymmetry transcription percentage was 99.3%.) [0086] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), 5ppm: 1.32 (t, 7.2Hz, 3H), 1.58 (dd, 23.6Hz, 6.9Hz, 3H), 4.26 (q, 7.2Hz, 2H), 5.00 (dq, 49.0Hz, 6.9Hz, 1H). 19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), 5ppm: -21.88 (dq, 48.9Hz, 24.4Hz, 1F) [0087] [EXAMPLE 5] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 3.50g (l5.00mmol, l.OOeq) of a primary alcohol derivative represented by the following formula, [Chemical Formula 27] 30.0mLof acetonitrile, 8.35g (82.52mmol, 5.50eq) of triethylamine, and 4.84g (30.02mmol, 2.00eq) of triethylamine tris(hydrogen fluoride) complex, followed by lowering the inside temperature to -40°C and then bubbling 7.86g (77.01mmol, 5.13eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 1 hr and 10 minutes. Stirring was further conducted at 60°C for 39 hours and 30 minutes. Conversion of the reaction was found by gas chromatography measurement to be 100%. 50.0mL of water were added to the reaction-terminated liquid, followed by concentration under reduced pressure, then adding 50.0mL of water to the concentrated residue, and then conducting an extraction one time with lOO.OmL of ethyl acetate. The recovered organic layer was dried with anhydrous sodium sulfate, followed by concentration under reduced pressure and vacuum drying, thereby obtaining 2.72g of a crude product of a monofluoromethyl derivative represented by the following formula, [Chemical Formula 28] as a dark brown color, oil-like substance. Selectivity of the crude product was found by gas chromatography measurement to be 69.4%. The crude product was found by internal standard method (internal standard substance: C6F6) of 19F-NMR to contain 3.45mmol of the monofluoromethyl derivative. The yield was 23%. Instrument data of the crude product of the obtained monofluoromethyl derivative are shown in the following. [0088] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), 5ppm: 0.90 (d, 6.8Hz, 3H), 1.08 (d, 6.8Hz, 3H), 2.44 (m, 1H), 4.24 (m, 1H), 4.76 (ddd, 46.6Hz, 9.5Hz, 4.8Hz, 1H), 5.01 (dt, 46.6Hz, 9.5Hz, 1H), 7.74 (Ar-H, 2H), 7.86 (Ar-H, 2H). 19F-NMR (standard substance-: C6F6, heavy solvent: CDCl3), δppm: -62.12 (dt, 13.3Hz, 46.6Hz, 1F). [0089] It is possible to produce the primary alcohol derivative of the raw material substrate from a commercial optically active valinol by referring to Protective Groups in Organic Synthesis, Third Edition, 1999, John Wiley & Sons, Inc. The obtained monofluoromethyl derivative can be converted to optically active l-isopropyl-2-fluoroethylamine without damaging optical purity by referring to the same book. [0090] [EXAMPLE 6] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 1.39g (7.98mmol, l.OOeq) of a primary alcohol derivative represented by the following formula, [Chemical Formula 29] as a brown color, oil-like substance. Selectivity of the crude product was found by gas chromatography measurement to be 98.6%. The yield was 16.0mL of acetonitrile, 4.45g (43.98mmol, 5.51eq) of triethylamine, and 2.58g (16.00mmol, 2.01eq) of triethylamine tris(hydrogen fluoride) complex, followed by lowering the inside temperature to -40°C and then bubbling 3.00g (29.39mmol, 3.68eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 19 hr and 15 minutes. Conversion of the reaction was found by gas chromatography measurement to be 100%. 10.0mL of water were added to the reaction-terminated liquid, followed by concentrating acetonitrile under reduced pressure and then conducting an extraction of the concentrated residue one time with 30.0mL of ethyl acetate. The recovered organic layer was washed with 10.0mL of saturated brine, followed by drying with anhydrous sodium sulfate, concentration under reduced pressure and vacuum drying, thereby obtaining 0.36g of a crude product of a monofluoromethyl derivative represented by the following formula, [Chemical Formula 30] 26%. Instrument data of the crude product of the obtained monofluoromethyl derivative are shown in the following. [0091] 1H-NMR (standard substance-' Me4Si, heavy solvent: CDCl3), δppm: 1.42-1.88 (m, 10H), 3.35-3.52 (m, 2H), 3.70-3.88 (m, 2H), 4.45 (dt, 46.8Hz, 6.1Hz, 2H), 4.56 (m, 1H). 19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), δppm: -56.37 (septet, 23.4Hz, 1F). [0092] It is possible to produce the primary alcohol derivative of the raw material substrate from a commercial optically active 1,4-butanediol by referring to Protective Groups in Organic Synthesis, Third Edition, 1999, John Wiley & Sons, Inc. The obtained monofluoromethyl derivative can be converted to 4-fluoro-1-butanol by referring to the same book. [0093] [EXAMPLE 7] A pressure-proof reaction vessel made of stainless steel (SUS) was charged with 1.58g (9.98mmol, l.OOeq) of a primary alcohol derivative represented by the following formula, [Chemical Formula 31] 20.0mLof acetonitrile, 5.57g (55.04mmol, 5.52eq) of triethylamine, and 3.22g (l9.97mmol, 2.00eq) of triethylamine tris(hydrogen fluoride) complex, followed by lowering the inside temperature to -40°C and then bubbling 2.04g (l9.99mmol, 2.00eq) of sulfuryl fluoride from a cylinder. The inside temperature was returned to room temperature, and stirring was conducted for 22 hr and 20 minutes. Conversion of the reaction was found by gas chromatography measurement to be 100%. 20.0mL of water were added to the reaction-terminated liquid, followed by conducting an extraction one time with 20.0mL of ethyl acetate. The recovered organic layer was washed with 20.0mL of water and then with 20.0mL of saturated brine, followed by drying with anhydrous sodium sulfate and concentration under reduced pressure, thereby obtaining a crude product of a monofluoromethyl derivative represented by the following formula, [Chemical Formula 32] as a brown color, oil-like substance. Selectivity of the crude product was found by gas chromatography measurement to be 94.2%. The crude product was found by internal standard method (internal standard substance: C6F6) of 19F-NMR to contain 2.10mmol of the monofluoromethyl derivative. The yield was 21%. Instrument data of the crude product of the obtained monofluoromethyl derivative are shown in the following. [0094] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), δppm: 0.89 (t, 6.8Hz, 3H), 1.20-1.45 (m, 14H), 1.60-1.70 (m, 2H), 4.44 (dt, 47.6Hz, 6.2Hz, 2H). 19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), 5ppm: -55.97 (septet, 23.8Hz, 1F). [0095] A commercial product was used as the primary alcohol derivative of the raw material substrate. WE CLAIM: 1. A dehydroxyfluorination agent comprising: sulfuryl fluoride (SO2F2); and an organic base that is free from a free hydroxyl group in the molecule. 2. A dehydroxyfluorination agent according to claim 1, wherein a ratio of the sulfuryl fluoride by mol number to the organic base is in a range of 1:5 to 5:1. 3. A dehydroxyfluorination agent according to claim 1 or claim 2, further comprising a hydrogen fluoride source added from outside of system, the hydrogen fluoride source being defined as hydrogen fluoride or a salt or complex formed between hydrogen fluoride and an organic base. 4. A dehydroxyfluorination agent according to claim 3, wherein a ratio of the sulfuryl fluoride by mol number to the hydrogen fluoride source (in terms of HF) added from the outside of the system is in a range of 1:10 to 3;1. 5. A dehydroxyfluorination agent according to any one of claim 1 to claim 4, wherein the organic base is selected from the group consisting of trimethylamine, triethylamine, diisopropylethylamine, tri-n-propylamine, pyridine, 2,3-lutidine, 2,4- lutidine, 2,5-lutidine, 2,6-lutidine, 3,4-lutidine, 3,5-lutidine, 2,3,4-collidine, 2,4,5- collidine, 2,5,6-collidine, 2,4,6-collidine, 3,4,5-collidine, and 3,5,6-collidine. 6. A dehydroxyfluorination agent according to any one of claim 1 to claim 5, further comprising an aprotic organic solvent. There is provided a novel, useful dehydroxyfluorination agent containing sulfuryl fluoride (SO2F2) and an organic base that is free from a free hydroxyl group in the molecule. According to the present dehydroxyfluorination agent, it is not necessary to use perfluoroalkanesulfonyl fluoride, which is not preferable in large-scale use, and it is possible to advantageously produce optically-active fluoro derivatives, which are important intermediates of medicines, agricultural chemicals and optical materials, for example, 4-fluoroproline derivatives, 2'-deoxy-2'-fluorouridine derivatives, optically-active α-fluorocarboxylate derivatives, and monofluoromethyl derivatives, even in large scale.

Full Text

TECHNICAL FIELD
[0001] The present invention relates to a novel dehydroxyfluorination
agent.
BACKGROUND OF THE INVENTION
[0002] "Dehydroxyfluorination reaction" for replacing hydroxyl group of a
hydroxyl group-containing compound with fluorine atom is an important
reaction in syntheses of fluorine-containing organic compounds. The
following are typical examples.
[0003] 1) a process (Patent Publication 1 and Patent Publication 2) in
which a substrate having a hydroxyl group is reacted with a
perfluoroalkanesulfonyl fluoride, such as perfluorobutanesulfonyl fluoride,
in the presence of a special, strongly basic, organic base, such as DBU
(1,8-diazabicyclo[5.4.0]undec-7-ene).
[0004] 2) a process (Non-patent Publication 1) in which a substrate having
a hydroxyl group is reacted with perfluorobutanesulfonyl fluoride in the
presence of an organic base, such as triethylamine, and "a salt or complex
comprising an organic base and hydrogen fluoride" such as triethylamine
tris(hydrogen fluoride) complex.
[0005] 3) a process (Patent Publications 3-6) for producing a fluoro
derivative by reacting a specific hydroxy derivative with
trifluoromethanesulfonyl fluoride in the presence of an organic base or in the
presence of an organic base and "a salt or complex comprising an organic
base and hydrogen fluoride" (such as triethylamine trisGrydrogen fluoride)
complex).
[0006] 4) a process (Non-patent Publication 2) in which a hydroxyl group is
converted into a fluorosulfate, followed by replacement with a fluorine anion.
Patent Publication 1: US Patent 5760255 specification

Patent Publication 2- US Patent 6248889 specification
Patent Publication 3: International Publication 2004/089968 Pamphlet
(Japanese Patent Application Publication 2004-323518)
Patent Publication 4- Japanese Patent Application Publication 2006-083163
Patent Publication 5: Japanese Patent Application Publication 2005-336151
Patent Publication 6: Japanese Patent Application Publication 2006008534
Non-patent Publication 1: Organic Letters (US), 2004, Vol. 6, No. 9, p.
14651468
Non-patent Publication 2: Tetrahedron Letters (UK), 1996, Vol. 37, No. 1, p.
17-20
SUMMARY OF THE INVENTION
[0007] In the processes of Patent Publication 1 and Patent Publication 2, it
was necessary to use a long-chain perfluoroalkanesulfonyl fluoride, which is
not preferable in large-scale use, and a high-price, special organic base. In
the dehydroxyfluorination reaction using a perfluoroalkanesulfonyl fluoride,
a perfluoroalkanesulfonic acid is stoichiometrically produced as a by-product
in the form of a salt of an organic base. Therefore, waste treatment of the
acid was a large problem in conducing the reaction in large scale. In
particular, long-chain perfluoroalkanesulfonic acid derivatives having a
carbon number of 4 or greater are pointed out to have long-term persistence
in environment and toxicity, and therefore their large-scale use is limited (for
example, see FARUMASHIA Vol. 40, No. 2, 2004 with respect to
perfluorooctanesulfonic acid derivatives).
[0008] Also in the process of Non-patent Publication 1, there was a similar
problem of using long-chain perfluorobutanesulfonyl fluoride.
[0009] On the other hand, the processes of Patent Publications 3-6 are
superior processes that are capable of avoiding problems of long-term
persistence in environment and toxicity, since they use
trifluoromethanesulfonyl fluoride having a carbon number of 1. The
industrial production amount of trifluoromethanesulfonyl fluoride is,
however, limited, as compared with perfluorobutanesulfonyl fluoride and

perfluorooctanesulfonyl fluoride. Therefore, its obtainment in large amount
was not necessarily easy.
[0010] The process of Non-patent Publication 2 was not a direct
fluorination reaction (see Scheme 1), due to its necessity of going through
imidazole sulfate in order to convert the hydroxy derivative to the
fluorosulfate.
[Chemical Formula 1]
Scheme 1

[0011] According to Non-patent Publication 1, it is disclosed therein that,
when the dehydroxyfluorination agent comprising trifluoromethanesulfonic
anhydride, triethylamine tris(hydrogen fluoride) complex and triethylamine
is used, gaseous trifluoromethanesulfonyl fluoride (boiling point: -21°C) is
formed in the reaction system, thereby not achieving an efficient
trifluoromethanesulfonylation of a hydroxyl group of the substrate, and that
a combination with high-boiling-point (64°C) perfluorobutanesulfonyl
fluoride (perfluorobutanesulfonyl fluoride, triethylamine tris(hydrogen
fluoride) complex and triethylamine) is preferable. This description clearly
indicates that low-boiling-point trifluoromethanesulfonyl fluoride is not
preferable as a perfluoroalkanesulfonyl fluoride of the dehydroxyfluorination
agent. Sulfuryl fluoride used in the present invention has a further lower
boiling point (-49.7°C). Thus, it has been totally unclear whether or not
that can preferably be used as the dehydroxyfluorination agent.
[0012] As mentioned hereinbefore, there has been a strong demand for a
novel dehydroxyfluorination means that is easy in large-scale operation, for
producing fluoro derivatives.
[0013] From the above viewpoint, the present inventors have conducted an
eager examination to find a novel dehydroxyfluorination means that is easy

in large-scale operation. As a result, we have found a novel
dehydroxyfluorination agent comprising sulfuryl fluoride (SO2F2) and an
organic base that is free from a free hydroxyl group in the molecule, thereby
reaching the present invention.
[0014] Sulfuryl fluoride (SO2F2) is a compound that is widely used as a
fumigant. There has been, however, no report of using the compound as a
dehydroxyfluorination agent.
[0015] By conducting a dehydroxyfluorination using a
dehydroxyfluorination agent of the present invention, it is possible to
continuously conduct a fluorosulfonylation and a fluorine substitution in one
reaction vessel without isolating a fluorosulfate that is a reaction
intermediate. As shown in Scheme 2, the characteristic of the present
invention is that a hydroxy derivative can be converted into a fluorosulfate
by using sulfuryl fluoride and that "a salt or complex comprising an organic
base and hydrogen fluoride", which has been stoichiometrically produced as
a by-product in the reaction system in the step of this fluorosulfonylation,
can be effectively used as a fluorine source of the fluorine substitution.
[0016] Furthermore, as shown in Scheme 3, in the case of using "the above
dehydroxyfluorination agent further comprising a hydrogen fluoride source
(it refers to hydrogen fluoride or a salt or complex formed between hydrogen
fluoride and an organic salt) added from the outside of the system", as
compared with the process shown in Scheme 2, it was also found that the
fluoro derivative can be obtained with high yield and selectivity.
[Chemical Formula 2]

[0017] In the present invention, sulfuryl fluoride has two reaction points to
the hydroxyl group. However, in the case of using 4-hydroxyproline
derivatives, which are particularly optically active hydroxy derivatives,
1-β-D-arabinofuranosyluracil derivatives, optically active
α-hydroxycarboxylate derivatives, and primary alcohol derivatives as
hydroxy derivatives, it was found that a disubstituted sulfate is almost not
given (see Scheme 4) and that the fluorine substitution proceeds well by
going through the target fluorosulfate. We have clarified that such problem
does not occur by perfluoroalkanesulfonyl fluoride and that sulfuryl fluoride
can preferably be used as a dehydroxyfluorination agent.
[Chemical Formula 4]

[0018] Furthermore, the present inventors have found that
stereochemistry of a fluoro derivative obtained by the reaction with sulfuryl
fluoride is inverted, in the case of using as the hydroxyl derivative an
optically active compound caused by chirality of the carbon atom that is
covalently bonded with the hydroxyl group. In the present
dehydroxyfluorination reaction, it is considered that the fluorosulfonylation
proceeds with maintenance of stereochemistry and the subsequent fluorine
substitution proceeds with inversion of stereochemistry. A
dehydroxyfluorination reaction accompanied with such inversion of
stereochemistry is also already disclosed in a process using a
perfluoroalkanesulfonyl fluoride of Patent Publication 2. However,
fluorosulfuric acid group is vastly inferior to perfluoroalkanesulfonic acid
group in leaving ability [Synthesis (Germany) 1982, Vol. 2, p. 85-126].
Therefore, it was unclear whether or not the reaction proceeds with high
asymmetry transcription percentage in a dehydroxyfluorination reaction,
using sulfuryl fluoride, of a chain substrate, which is difficult in control of
stereochemistry, particularly an optically active orhydroxycarboxylate
derivative. In contrast with this, the present inventors have found that a
dehydroxyfluorination using sulfuryl fluoride of the present invention
proceeds well under a very mild reaction condition and that an optically
active α-fluorocarboxylate derivative, which is extremely high in optical
purity, is obtained by the reflection of optical purity of the optically active
orhydroxycarboxylate derivative, which is used as the raw material
substrate.
[0019] Furthermore, it was unclear whether or not fluorosulfates that are
obtained by conversion of 4-hydroxyproline derivative and

1-β-D-arabinofuranosyluracil derivative through fluorosulfonylation and
that correspond to the respective raw material substrates have sufficient
leaving abilities. In contrast with this too, the present inventors have found
that a dehydroxyfluorination reaction using sulfuryl fluoride of the present
invention can preferably be used as the process for producing 4-fluoroproline
derivative and 2'deoxy2'-fluorouridine derivative.
DETAILED DESCRIPTION
[0020] Advantageous points of the dehydroxyfluorination agent of the
present invention are described in the following, as compared with prior art.
[0021] Relative to the processes of Patent Publication 1, Patent Publication
2 and Non-patent Publication 1, it is not necessary to use
perfluoroalkanesulfonyl fluorides that are problematic in waste treatment,
long-term persistence in environment and toxicity, and it is possible in the
present invention to use sulfuryl fluoride, which is widely used as a
fumigant.
[0022] In the case of conducting a dehydroxyfluorination reaction using a
dehydroxyfluorination agent of the present invention, fluorosulfuric acid is
stoichiometrically produced as a salt of an organic base. It is, however,
possible to easily treat the acid into fluorite (CaF2) as a final waste. It is
thus extremely preferable for a fluorination reaction in large scale.
[0023] Furthermore, the perfluoroalkyl moiety of perfluoroalkanesulfonyl
fluoride is at last not incorporated into the target product. One having a
less fluorine content is advantageous in atomic economy, as long as it has
sufficient sulfonylation ability and leaving ability. From such a viewpoint
too, sulfuryl fluoride is vastly superior.
[0024] In a dehydroxyfluorination agent of the present invention, it is not
necessary to use a high-price, special organic base such as DBU, and it is
possible to use a low-price organic base, such as triethylamine, that is
common in large-scale production.
[0025] Relative to the process of Non-patent Publication 2, it is not
necessary to go through imidazole sulfate. In the present invention, it is

possible to directly convert a hydroxy derivative to a fluorosulfate by using
sulfuryl fluoride.
[0026] Furthermore, a new advantageous effect of the invention has been
found by using sulfuryl fluoride. In a dehydroxyfluorination reaction using
a perfluoroalkanesulfonyl fluoride, a salt of a perfluoroalkanesulfonic acid
and an organic base is stoichiometrically contained in the
reaction-terminated liquid. The salt, particularly a salt derived from a
perfluoroalkanesulfonic acid having a carbon number of 4 or greater, has an
extremely high solubility in organic solvent. We thus have found that there
is a problem that it is not possible to effectively remove the salt and thereby
it imposes a burden on the purification operation, even if conducting a
post-treatment operation that is generally used in organic syntheses, such as
washing of organic layer with water or alkali aqueous solution.
Furthermore, a salt of perfluoroalkanesulfonic acid and organic base may act
as an acid catalyst in some cases. Thus, it was necessary to efficiently
remove the salt in order to produce a compound having an acid-labile
functional group. Actually, if a large amount of a salt of
perfluorobutanesulfonic acid and organic base is contained in a distillation
purification of a crude product of 4-fluoroproline derivative, in which the
protecting group of the secondary amino group is a tert-butoxycarbonyl (Boc)
group, debutoxycarbonylation reaction is found considerably. Thus, it was
not possible to recover the target product with good yield. On the other
hand, a salt of fluorosulfuric acid and organic base, which is produced as a
by-product in the present invention, is extremely high in solubility in water.
Therefore, it can perfectly be removed by washing the organic layer with
water or alkali aqueous solution. Since it does almost not impose a burden
on the purification operation, it was found to be extremely preferable for a
fluorination reaction in large scale.
[0027] A dehydroxyfluorination agent having characteristics disclosed in
the present invention has not been disclosed at all in related technical fields.
It is extremely useful as a dehydroxyfluorination agent in large scale, since it

is very high in selectivity and does almost not produce as by-products
impurities that are difficult in separation. In particular, it can extremely
preferably be used for a large-scale production process of optically active
fluoro derivatives, which are important intermediates of medicines,
agricultural chemicals and optical materials, specifically 4-fluoroproline
derivatives, 2'-deoxy-2'-fluorouridine derivatives and optically active
α-fiuorocarboxylate derivatives, and monofluoromethyl derivatives. It is
capable of remarkably efficiently producing them, as compared with
conventional production processes.
[0028] In the following, a dehydroxyfluorination agent of the present
invention is described in more detail.
[0029] It is possible to prepare a dehydroxyfluorination agent of the present
invention by introducing sulfuryl fluoride into a container in which an
organic base exists. In order to further improve reactivity, it is also possible
to further add a hydrogen fluoride source (it refers to hydrogen fluoride or a
salt or complex formed between hydrogen fluoride and an organic base) from
the outside of the system. Furthermore, it is also possible to add an aprotic
organic solvent in order to make the reaction proceed more smoothly.
[0030] Herein, the container is desirably a pressure-proof airtight container,
since sulfuryl fluoride is in gas under ordinary temperature and ordinary
pressure.
[0031] The order of adding the reagents and the preparation method are
not particularly limited, (i) It is possible to prepare a dehydroxyfluorination
agent of the present invention by previously placing an organic base that is
free from a free hydroxyl group in the molecule (and, according to need, "a
hydrogen fluoride source added from the outside of the system" and an
aprotic organic solvent) in a container, then sealing it, and introducing
gaseous sulfuryl fluoride thereinto, (ii) It is also possible to previously place
each component of the above, except sulfuryl fluoride, and the reaction raw
material (the hydroxy derivative) into a container and successively or
continuously introduce sulfuryl fluoride thereinto. In the case of (ii), the

dehydroxyfluorination reaction starts at the same time when the
dehydroxyfluorination agent is prepared. Like (ii), to prepare a
dehydroxyfluorination agent of the present invention in the reaction system
(in situ) is simpler and easier in handling. On the other hand, in large-scale
production, it is practical in some cases to introduce sulfuryl fluoride in
liquid state under pressurized condition.
[0032] The organic base used for a dehydroxyfluorination agent of the
present invention is an organic base that is free from a free hydroxyl group
in the molecule. In case that a free hydroxyl group exists in a part of the
base molecule, it can preferably be used by protecting those hydroxyl groups
with various protecting groups. However, as compared with the use by
protecting such base, it is economically more preferable to directly use one
that is generally available as an organic base with low price. In particular,
a base is preferable that is selected from the group consisting of
trimethylamine, triethylamine, diisopropylethylamine, tri-n-propylamine,
pyridine, 2,3-lutidine, 2,4-lutidine, 2,5-lutidine, 2,6-lutidine, 3,4-lutidine,
3,5'lutidine, 2,3,4-collidine, 2,4,5-collidine, 2,5,6'collidine, 2,4,6-collidine,
3,4,5-collidine, 3,5,6-collidine, and the like. Particularly, triethylamine,
diisopropylethylamine, pyridine, 2,4-lutidine, 2,6-lutidine, 3,5-lutidine, and
2,4,6-collidine are preferable.
[0033] The present inventors have found that reactivity of the
dehydroxyfluorination improves strikingly by further adding "hydrogen
fluoride source" to the dehydroxyfluorination agent of the present invention.
Herein, "hydrogen fluoride source" refers to hydrogen fluoride or a salt or
complex formed between hydrogen fluoride and an organic base.
[0034] As shown in Scheme 2, in the dehydroxyfluorination reaction of the
present invention, firstly in the fluorosulfate formation, an equimolar
amount of hydrogen fluoride (this hydrogen fluoride may form a salt or
complex with the organic base) is generated in the system. This hydrogen
fluoride becomes a fluorine source in the subsequent fluorine substitution,
and it conducts a nucleophilic attack against the fluorosulfate of the reaction

intermediate. With this, the fluorine substitution proceeds. This fluorine
substitution is markedly accelerated when hydrogen fluoride is in an
excessive condition by the addition of the hydrogen fluoride source from the
outside of the system. In particular, it was found that a great effect is
generated in the case of dehydroxyfluorinating a hydroxy derivative that is
low in reactivity.
[0035] In a dehydroxyfluorination agent of the present invention, the ratio
of sulfuryl fluoride by mol number to the organic base is not particularly
limited. However, as shown in Scheme 2, the ratio of sulfuryl fluoride,
which is consumed in the dehydroxyfluorination reaction, by mol number to
the organic base is 1:1 in theory. Therefore, in principle, it suffices that the
ratio of both is about 1:1. However, it is possible in some cases to obtain a
higher reactivity by excessively using one of both. Specifically, the ratio of
sulfuryl fluoride by mol number to the organic base is preferably in a range
of roughly 5:1-1:5.
[0036] Furthermore, in the dehydroxyfluorination agent of the present
invention, in the case of adding "hydrogen fluoride or a salt or complex
formed between hydrogen fluoride and an organic base (e.g., triethylamine
tris(hydrogen fluoride) complex)" as a hydrogen fluoride source from the
outside of the system, the ratio of sulfuryl fluoride by mol number to the
above hydrogen fluoride source (in terms of HF) is preferably in a range of
roughly 3:1-1:10, more preferably in a range of 1:1-1:10. If the mol number
(in terms of HF) of the hydrogen fluoride source is less than 1/3 of the mol
number of sulfuryl fluoride, the effect of positively adding it is low. If it is
greater than 10 times that, it becomes disadvantageous in economy and
production.
[0037] As these organic bases used for "the salt or complex comprising an
organic base and hydrogen fluoride" added from the outside of the system, it
is possible to preferably use any of the types mentioned as "the organic base
that is free from a free hydroxyl group in the molecule", which is an essential
element of the present invention. This organic base in the salt or complex

may be of a type that is different from the organic base that is an essential
element of the present invention, but being the same type is simple. Still
triethylamine is one of particularly preferable ones.
[0038] In the case of using a salt or complex comprising an organic base
and hydrogen fluoride, the molar ratio of the organic base to the hydrogen
fluoride in this salt or complex is in a range of 100:1-1:100, preferably in a
range of 50:1-1:50 in general, more preferably in a range of 25:1-1:25 in
particular. Furthermore, it is extremely convenient to use "a complex
comprising 1 mol of triethylamine and 3 mols of hydrogen fluoride" and "a
complex comprising ~30% (-10 mol%) of pyridine and -70% (~90mol%) of
hydrogen fluoride", which are placed on sale from Aldrich (Aldrich,
2003-2004 Comprehensive Catalogue).
[0039] Apart from the above-mentioned organic base, it is desirable to
further add an aprotic organic solvent in order to have a mutual affinity
between sulfuryl fluoride and the organic base in a dehydroxyfluorination
agent of the present invention. As such aprotic organic solvent, it is
possible to mention aliphatic hydrocarbon series such as n-hexane,
cyclohexane and n-heptane; aromatic hydrocarbon series such as benzene,
toluene, xylene and mesitylene; halogenated hydrocarbon series such as
methylene chloride, chloroform and 1,2'dichloroethane; ether series such as
diethyl ether, tetrahydrofuran and tert-butyl methyl ether; ester series such
as ethyl acetate and n-butyl acetate; amide series such as
N,N-dimethylformamide, N,N-dimethylacetamide and N-methylpyrrolidone;
nitrile series such as acetonitrile and propionitrile; dimethylsulfoxide,' and
the like. Of these, n-heptane, toluene, mesitylene, methylene chloride,
tetrahydrofuran, ethyl acetate, N,N-dimethylformamide,
N,N-dimethylacetamide, acetonitrile, propionitrile, and dimethylsulfoxide
are preferable. In particular, toluene, mesitylene, methylene chloride,
tetrahydrofuran, N,N-diemethylformamide, and acetonitrile are more
preferable. It is possible to use these reaction solvents alone or in
combination.

[0040] The amount of the aprotic organic solvent is not particularly limited.
It suffices to use 0.1L (liter) or greater, preferably 0.1-20L in general, more
preferably 0.1-10L in particular, relative to 1 mole of sulfuryl fluoride.
[0041] By using a dehydroxyfluorination agent of the present invention, it
is possible to continuously conduct the fluorosulfonylation and the fluorine
substitution in one reactor without separation of the fluorosulfate, which is a
reaction intermediate.
[0042] Furthermore, in the fluorosulfonylation, stereochemistry of the
hydroxyl group is maintained, and stereochemistry is inverted in the
subsequent fluorine substitution. Therefore, 4-fluoroproline derivative in
4S/2R configuration is obtained from 4-hydroxyproline derivative in 4R/2R
configuration. Similarly, 4R/2R configuration from 4S/2R configuration,
4S/2S configuration from 4R/2S configuration, and 4R/2S configuration from
4S/2S configuration. Optically active crfluorocarboxylate derivative in S
configuration at α-position is obtained from optically active
α-hydroxycarboxylate derivative in R configuration at α-position. Similarly,
R configuration at crposition is obtained from S configuration at a-position
with good selectivity.
[0043] [Regarding Hydroxy Derivative]
According to a dehydroxyfluorination agent of the present invention,
it is possible to substitute F atom for OH group of various hydroxy
derivatives (they refer to compounds having at least one free hydroxyl group
in the molecule). In the following, a hydroxy derivative, to which a
dehydroxyfluorination agent of the present invention can be applied, is
described.
[0044] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite a hydroxy
derivative represented by the general formula [1],
[Chemical Formula 5]

[in the formula, each of R, R1 and R2 independently represents a hydrogen
atom, alkyl group, substituted alkyl group, aromatic ring group, or
alkoxycarbonyl group]. By dehydroxyfluorinating the present compound, it
is possible to obtain a fluoro derivative represented by the general formula
[2],
[Chemical Formula 6]

[in the formula, R, R1 and R2 are defined as in the general formula [1]].
[0045] When R, R1 and R2 of the hydroxyl derivative represented by the
general formula [1] are alkyl groups, substituted alkyl groups, aromatic ring
groups or alkoxycarbonyl groups other than hydrogen atoms, they also can
have an optically active moiety caused by chirality of carbon atom, axis and
the like. In these cases, stereochemistry of the optically active moiety is
maintained through the fluorination reaction of the present invention.
[0046] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite a hydroxy
derivative represented by the general formula [la],
[Chemical Formula 7]

[In the formula, each of R, R1 and R2 independently represents a hydrogen
atom, alkyl group, substituted alkyl group, aromatic ring group, or
alkoxycarbonyl group. The alkyl group is defined as being a C1C16

straight-chain or branched alkyl group. The substituted alkyl group is
defined as being an alkyl group, in which a halogen atom, lower alkoxy group,
lower haloalkoxy group, lower alkylamino group, lower alkylthio group,
cyano group, aminocarbonyl group (CONH2), unsaturated group, aromatic
ring group, nucleic acid base, aromatic-ring oxy group, aliphatic heterocyclic
group, protected hydroxyl group, protected amino group, protected thiol
group, or protected carboxyl group has been substituted therefor by any
number and by any combination on any carbon atom of the alkyl group.
Any carbon atoms themselves of any two alkyl groups or substituted alkyl
groups may form a covalent bond to have an aliphatic ring, and carbon atoms
of the aliphatic ring may be partially replaced with nitrogen atom or oxygen
atom to have an aliphatic heterocyclic ring. The aromatic ring group is
defined as being an aromatic hydrocarbon group or aromatic heterocyclic
group containing oxygen atom, nitrogen atom or sulfur atom. The
alkoxycarbonyl group is defined as being an alkoxycarbonyl group
comprising an C1-C12 straight-chain or branched alkoxy group, and any
carbon atoms themselves of the alkoxy group and of any alkyl group or
substituted alkyl group may form a covalent bond to have a lactone ring.].
By dehydroxyfluorinating the present compound, it is possible to obtain a
fluoro derivative represented by the general formula [2a],
[Chemical Formula 8]

[in the formula, R, R1 and R2 are defined as in the general formula [la]].
[0047] The substituted alkyl group of R, R1 and R2 of the hydroxy derivative
represented by the general formula [la] is defined as being "an alkyl group,
in which a halogen atom of fluorine, chlorine, bromine and iodine; lower
alkoxy group such as methoxy group, ethoxy group and propoxy group; lower
haloalkoxy group such as fluoromethoxy group, chloromethoxy group and

bromomethoxy group; lower alkylamino group such as dimethylamino group,
diethylamino group and dipropylamino group,' lower alkylthio group such as
methylthio group, ethylthio group and propylthio group; cyano group;
aminocarbonyl group (CONH2); unsaturated group such as alkenyl group
and alkynyl group; aromatic ring group such as phenyl group and naphthyl
group; nucleic acid base such as adenine residue, guanine residue,
hypoxanthine residue, xanthine residue, uracil residue, thymine residue and
cytosine residue; aromaticring oxy group such as phenoxy group and
naphthoxy group,' aliphatic heterocyclic group such as piperidyl group,
piperidino group and morpholyl group; protected hydroxyl group, protected
amino group, protected thiol group, protected carboxyl group, or the like has
been substituted therefor by any number and by any combination on any
carbon atom of the alkyl group".
[0048] In the present specification, each of the following terms is used as
having the following meaning. "Lower" means C1-C6 straight-chain or
branched. In case that "unsaturated group" is a double bond, it can be in a
geometrical isomerism of either E configuration or Z configuration.
"Aromatic ring group" also can be an aromatic heterocyclic group (containing
a condensed skeleton) containing oxygen atom, nitrogen atom, sulfur atom
and the like, such as furyl group, pyrrolyl group and thienyl group, other
than aromatic hydrocarbon groups. "Nucleic acid base" can be protected
with a protecting group that is generally used in the field of syntheses of
nucleic acid related substances (For example, as a protecting group of
hydroxyl group, it is possible to mention acyl groups such as acetyl group and
benzoyl group; alkyl groups such as methoxymethyl group and allyl group;
and aralkyl groups such as benzyl group and triphenylmethyl group. As a
protecting group of amino group, it is possible to mention acyl groups such as
acetyl group and benzoyl group and aralkyl groups such as benzyl group.
Furthermore, halogen atom, lower alkyl group, lower alkoxy group and the
like can be substituted in these protecting groups.). Furthermore, hydrogen
atom, hydroxyl group and amino group of "nucleic acid base" can be replaced

with hydrogen atom, amino group, halogen atom, lower alkyl group, lower
alkenyl group nitro group and the like. As "protecting groups of hydroxyl
group, amino group, thiol group and carboxyl group", it is possible to use
protecting groups and the like described in Protective Groups in Organic
Synthesis, Third Edition, 1999, John Wiley & Songs, Inc. In "unsaturated
group", "aromatic ring group", "aromatic ring oxy group" and "aliphatic
heterocyclic group", it is possible to substitute lower alkyl group, halogen
atom, lower haloalkyl group, lower alkoxy group, lower haloalkoxy group,
lower alkylamino group, lower alkylthio group, cyano group, aminocarbonyl
group, protected hydroxyl group, protected amino group, protected thiol
group, protected carboxyl group, and the like.
[0049] Alkyl group and substituted alkyl group of R, R1 and R2 of the
hydroxy derivative represented by the general formula [la] also can be an
aliphatic ring, such as cyclopentane ring and cyclohexane ring, by the
formation of a covalent bond by any carbon atoms of any two alkyl groups or
substituted alkyl groups. They also can be an aliphatic heterocyclic ring,
such as pyrrolidine ring (also containing a protected secondary amino group),
piperidine ring (also containing a protected secondary amino group), oxolane
ring and oxane ring, in which carbon atoms of the aliphatic ring have been
partially replaced with nitrogen atoms or oxygen atoms.
[0050] Aromatic ring group of R, R1 and R2 of the hydroxy derivative
represented by the general formula [la] is defined as being "an aromatic
hydrocarbon group, such as phenyl group, naphthyl group and anthryl group,
or aromatic heterocyclic group containing oxygen atom, nitrogen atom, sulfur
atom or the like, such as furyl group, pyrrolyl group, thienyl group,
benzofuryl group, indolyl and benzothienyl group. In these aromatic
hydrocarbon groups and aromatic heterocyclic groups, it also possible to
substitute lower alkyl group, halogen atom, lower haloalkyl group, lower
alkoxy group, lower haloalkoxy group, lower alkylamino group, lower
alkylthio group, cyano group, aminocarbonyl group, unsaturated group,
aromatic ring group, aromatic ring oxy group, aliphatic heterocyclic group,

protected hydroxyl group, protected amino group, protected thiol group,
protected carboxyl group, and the like.
[0051] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite an optically active
hydroxy derivative represented by the general formula [3],
[Chemical Formula 9]

[In the formula, each of R and R1 is independently an alkyl group,
substituted alkyl group, or alkoxycarbonyl group. * represents an
asymmetric carbon (R and R' do not take the same substituent). The alkyl
group is defined as being a C1-C16 straight-chain or branched alkyl group.
The substituted alkyl group is defined as being an alkyl group, in which a
halogen atom, lower alkoxy group, lower haloalkoxy group, lower alkylamino
group, lower alkylthio group, cyano group, aminocarbonyl group (CONH2),
unsaturated group, aromatic ring group, nucleic acid base, aromatic-ring oxy
group, aliphatic heterocyclic group, protected hydroxyl group, protected
amino group, protected thiol group, or protected carboxyl group has been
substituted therefor by any number and by any combination on any carbon
atom of the alkyl group. Any carbon atoms themselves of two alkyl groups
or substituted alkyl groups may form a covalent bond to have an aliphatic
ring, and carbon atoms of the aliphatic ring may be partially replaced with
nitrogen atom or oxygen atom to have an aliphatic heterocyclic ring. The
alkoxycarbonyl group is defined as being an alkoxycarbonyl group
comprising an C1-C12 straight-chain or branched alkoxy group, and any
carbon atoms themselves of the alkoxy group and of any alkyl group or
substituted alkyl group may form a covalent bond to have a lactone ring.
Stereochemistry of the carbon atom, to which the hydroxyl group is
covalently bonded, is inverted through the reaction.] By

dehydroxyfluorinating the present compound, it is possible to obtain an
optically active fluoro derivative represented by the general formula [4],
[Chemical Formula 10]

[In the formula, R, R1 and * are defined as in the general formula [3]].
[0052] The dehydroxyfluorination reaction of the present invention
becomes particularly effective for the production of high-optical-purity fluoro
derivatives, which are required for important intermediates of medicines,
agricultural chemicals and optical materials. In order to maximize this
effect, the selection of the raw material substrate is important. Specifically,
although it can be applied to optically active tertiary alcohol derivatives,
which are sterically bulky, optically active secondary alcohol derivatives
(corresponding to optically active hydroxy derivatives represented by the
general formula [3]), which can be expected to have a high asymmetry
transcription percentage, are still more preferable. Furthermore, the
substituents of the optically active secondary alcohol derivative
(corresponding to R and R' of the optically active hydroxy derivative
represented by the general formula [3]) are preferably alkyl group,
substituted alkyl group and alkoxycarbonyl group, as compared with
aromatic ring groups, which are expected to be accompanied with a partial
racemization by going through a transition state, such as the benzyl-position
carbonium ion, in the course of the fluorine substitution of the fluorosulfate
as the reaction intermediate.
[0053] Due to the usefulness of the product to be obtained, the carbon
number of the alkyl group is generally preferably 1 to 14, particularly more
preferably 1 to 12. The substituents of the substituted alkyl group are
preferably nucleic acid base, protected hydroxyl group, protected amino
group, and protected carboxyl group. It is preferable that two alkyl groups

or substituted alkyl groups take an aliphatic heterocyclic ring. The carbon
number of the alkoxy group of the alkoxycarbonyl group is generally
preferably 1 to 10, particularly more preferably 1 to 8.
[0054] Furthermore, stereochemistry of the asymmetric carbon of the
optically active secondary alcohol derivative (corresponding to the optically
active hydroxy derivative represented by the general formula [3]) can be R
configuration or S configuration. Enantiomer excess ratio (%ee) is not
particularly limited. It suffices to use one having 90%ee or greater. In
general, 95%ee or greater is preferable, and particularly 97%ee is more
preferable.
[0055] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite a 4-hydroxyproline
derivative represented by the general formula [5],
[Chemical Formula 11]

[In the formula, R3 represents a protecting group of the secondary amino
group, R4 represents a protecting group of the carboxyl group, * represents
an asymmetric carbon, and stereochemistry of the 4-position is inverted
through the reaction, and stereochemistry of the 2-position is maintained.]
By dehydroxyfluorinating the present compound, it is possible to obtain a
4-fluoroproline derivative represented by the general formula [6],
[Chemical Formula 12]

[In the formula, R3, R4 and * are defined as in the general formula [5]].
[0056] As the protecting group R3 of the secondary amino group of the
4-hydroxyproline derivative represented by the general formula [5], it is
possible to mention benzyloxycarbonyl (Z) group, tert-butoxycarbonyl (Boc)
group, 9-fluorenylmethoxycarbonyl (Fmoc) group, 3-nitro-2-pyridinesulfenyl
(Npys) group, p-methoxybenzyloxycarbonyl [Z(MeO)] group, and the like.
Of these, benzyloxycarbonyl (Z) group and tert-butoxycarbonyl (Boc) group
are preferable, and particularly tert-butoxycarbonyl (Boc) group is more
preferable.
[0057] As the protecting group R4 of the carboxyl group of the
4-hydroxyproline derivative represented by the general formula [5], it is
possible to mention methyl (Me) group, ethyl (Et) group, tert-butyl (t-Bu)
group, trichloroethyl (Tce) group, phenacyl (Pac) group, benzyl (Bzl) group,
4-nitrobenzyl [Bzl(4"NO2)] group, 4-methoxybenzyl [Bzl(4"MeO)] group, and
the like. Of these, methyl (Me) group, ethyl (Et) group and benzyl (Bzl)
group are preferable, and particularly methyl (Me) group and ethyl (Et)
group are more preferable.
[0058] It is possible to produce the 4-hydroxyproline derivative represented
by the general formula [5] from a commercial optically active
4-hydroxyproline by referring to 4th Edition Jikken Kagaku Koza 22 Organic
Synthesis IV Acid, Amino acid, Peptide (Maruzen, 1992, p. 193-309).
Depending on a combination of the protecting group R3 of the secondary
amino group and the protecting group R4 of the carboxyl group, there are
commercial products, and it is also possible to use these. Of the
4-hydroxyproline derivative represented by the general formula [5], it is
possible to easily convert a hydrochloride of optically active 4-hydroxyproline
methyl ester into one in which the protecting group R3 of the secondary
amino group is a tert-butoxycarbonyl (Boc) group and in which the protecting
group R4 of the carboxyl group is a methyl (Me) group, in accordance with
Tetrahedron Letters (United Kingdom), 1988, Vol. 39, No. 10, p. 1169-1172.
[0059] As stereochemistry of the asymmetric carbon of the

4-hydroxyproline derivative represented by the general formula [5], each of
2-position and 4-position can independently take R configuration or S
configuration. As a combination of stereochemistry, there is 4R/2R form,
4S/2R form, 4R/2S form or 4S/2S form. Enantiomer excess ratio (%ee) or
diastereomer excess ratio (%de) of each stereoisomer is not particularly
limited. It suffices to use 90%ee or 90%de or greater, normally preferably
95%ee or 95%de or greater, particularly more preferably 97%ee or 97%de or
greater.
[0060] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite a
1-β-D-arabinofuranosyluracil derivative represented by the general formula
[7],
[Chemical Formula 13]

[In the formula, each of R5 and R6 independently represents a protecting
group of the hydroxyl group.]. By dehydroxyfluorinating the present
compound, it is possible to obtain a 2'-deoxy-2'-fluorouridine derivative
represented by the general formula [8],
[Chemical Formula 14]

[In the formula, R5 and R6 are defined as in the general formula [7].].
[0061] As the protecting groups R5 and R6 of the hydroxyl groups of the
1-β-D-arabinofuranosyluracil derivative represented by the general formula
[7], it is possible to mention trithyl group (triphenylmethyl group),
tetrahydropyranil group (THP group), and tetrahydrofuranyl group (THF
group). Of these, tetrahydropyranil group (THP group), and
tetrahydrofuranyl group (THF group) are preferable, and particularly
tetrahydropyranil group (THP group) is more preferable. It is possible to
produce 1-β-D-arabinofuranosyluracil derivative represented by the general
formula [7] by referring to Chem. Pharm. Bull. (Japan), 1994, Vol. 42, No. 3,
p. 595-598 and Khim. Geterotsikl. Soedin. (Russia), 1996, No. 7, p. 975-977.
It is possible to obtain one, in which hydroxyl groups of 3'-position and
5'-position are selectively protected, by following the processes of these
publications.
[0062] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite an optically-active,
a-hydroxycarboxylate derivative represented by the general formula [9],
[Chemical Formula 15]

[In the formula, R7 represents a C1-C12 alkyl group or substituted alkyl group,
R8 represents a C1-C8 alkyl group, any carbon atoms themselves of the alkyl

group or of the substituted alkyl group of R7 and R8 may form a covalent
bond to have a lactone ring, * represents an asymmetric carbon, and
stereochemistry of the orposition is inverted through the reaction.]. By
dehydroxyfluorinating the present compound, it is possible to obtain an
optically-active, α-fluorocarboxylate derivative represented by the general
formula [10],
[Chemical Formula 16]

[In the formula, R7, R8 and * are defined as in the general formula [9].].
[0063] As R7 of the optically active orhydroxycarboxylate derivative
represented by the general formula [9], it is possible to mention methyl
group, ethyl group, propyl group, butyl group, amyl group, hexyl group,
heptyl group, octyl group, nonyl group, decyl group, undecyl group, and
lauryl group. The alkyl group having a carbon number of 3 or greater can
be straight-chain or branched. On any carbon atom of the alkyl group, it is
possible to substitute one or any combination of two of aromatic hydrocarbon
groups such as phenyl group and naphthyl group, unsaturated hydrocarbon
groups such as vinyl group, C1-C6 straight-chain or branched alkoxy groups,
aryloxy groups such as phenoxy group, halogen atoms (fluorine, chlorine,
bromine and iodine), protected carboxyl groups, protected amino groups, or
protected hydroxyl groups. As the protecting groups of the carboxyl group,
amino group and hydroxyl group, similar to the above, it is possible to use
protecting groups described in Protective Groups in Organic Synthesis,
Third Edition, 1999, John Wiley & Sons, Inc. Specifically, it is possible to
mention ester group and the like as the protecting group of the carboxyl
group. It is possible to mention benzyl group, acyl groups (acetyl group,
chloroacetyl group, benzoyl group, 4-methylbenzoyl group and the like), and
phthaloyl group, and the like as the protecting group of the amino group. It
is possible to mention benzyl group, 2-tetrapyranil group, acyl groups (acetyl

group, chloroacetyl group, benzoyl group, 4-methylbenzoyl group and the
like), silyl groups (trialkylsilyl group, alkylarylsilyl group and the like), and
the like, as the protecting group of the hydroxyl group. In particular, it is
possible to mention a protecting group or the like that forms
2,2-dimethy1-1,3-dioxolane, as the protecting group of the 1,2-dihydroxy
group.
[0064] Although the production process, which is the target of the present
invention, can be used even in case that R7 of the optically active
orhydroxycarboxylate derivative represented by the general formula [9] is an
aromatic hydrocarbon group, optical purity of the target product, optically
active a-fluorocarboxylate derivative (R7 = an aromatic hydrocarbon group)
represented by the general formula [10], lowers significantly, as compared
with a case that R7 is an alkyl group or substituted alkyl group. Therefore,
an alkyl group or substituted alkyl group is preferable as R7 of the optically
active orhydroxycarboxylate derivative represented by the general formula
[9].
[0065] As R8 of the optically active a-hydroxycarboxylate derivative
represented by the general formula [9], it is possible to mention methyl
group, ethyl group, propyl group, butyl group, amyl group, hexyl group,
heptyl group, and octyl group. The alkyl group having a carbon number of 3
or greater can be straight-chain or branched.
[0066] Stereochemistry of the asymmetric carbon of the optically active
orhydroxycarboxylate derivative represented by the general formula [9] can
be R configuration or S configuration. Enantiomer excess ratio (%ee) is not
particularly limited. It suffices to use one having 90%ee or greater. In
general, 95%ee or greater is preferable, and particularly 97%ee is more
preferable.
[0067] The optically active orhydroxycarboxylate derivative represented by
the general formula [9] can be produced similarly from various, commercial,
optically-active, oramino acids by referring to Synthetic Communications
(US), 1991, Vol. 21, No. 21, p. 2165-2170. A commercial product was used as

(S)-ethyl lactate used in the Examples.
[0068] As a hydroxy derivative, to which a dehydroxyfluorination agent of
the present invention can be applied, it is possible to cite a primary alcohol
derivative represented by the general formula [11],
[Chemical Formula 17]

[In the formula, R represents an alkyl group or substituted alkyl group, the
alkyl group is defined as being a C1-C16 straight-chain or branched alkyl
group, and the substituted alkyl group is defined as being an alkyl group, in
which a halogen atom, lower alkoxy group, lower haloalkoxy group, lower
alkylamino group, lower alkylthio group, cyano group, aminocarbonyl group
(CONH2), unsaturated group, aromatic ring group, nucleic acid base,
aromatic-ring oxy group, aliphatic heterocyclic group, protected hydroxyl
group, protected amino group, protected thiol group, or protected carboxyl
group has been substituted therefor by any number and by any combination
on any carbon atom of the alkyl group.]. By dehydroxyfluorinating the
present compound, it is possible to obtain a monofluoromethyl derivative
represented by the general formula [12],
[Chemical Formula 18]

[In the formula, R is defined as in the general formula [11].].
[0069] In the development of medicines having new effectiveness,
"monofluoromethyl group" is recognized as being an important motif. Thus,
primary alcohol derivatives (corresponding to the primary alcohol derivative
represented by the general formula [11]), which can efficiently produce

monofluoromethyl derivatives (corresponding to the monofluoromethyl
derivative represented by the general formula [12]), are also preferable
substrates.
[0070] The optically active hydroxy derivative represented by the general
formula [3], the 4-hydroxyproline derivative represented by the general
formula [5], 1-β-D-arabinofuranosyluracil derivative represented by the
general formula [7], the optically active orhydroxycarboxylate derivative
represented by the general formula [9], and the primary alcohol derivative
represented by the general formula [11] are particularly preferable as the
hydroxy derivative represented by the general formula [1].
[0071] [Reaction Conditions of Dehydroxyfluorination]
The amount of sulfuryl fluoride (SO2F2) used in the
dehydroxyfluorination agent of the present invention relative to 1mol of the
hydroxy derivative is not particularly limited. It suffices to use lmol or
greater, preferably 1-10 moles in general, and more preferably 1-5 moles in
particular.
[0072] The amount of the organic base used in the dehydroxyfluorination of
the present invention relative to lmol of the hydroxy derivative is not
particularly limited. It suffices to use lmol or greater, preferably 1-20
moles in general, more preferably 1-10 moles in particular.
[0073] The amount of the hydrogen fluoride source (it refers to hydrogen
fluoride or a salt or complex formed between hydrogen fluoride and organic
base) used in the dehydroxyfluorination agent of the present invention
relative to lmol of the hydroxy derivative is not particularly limited. It
suffices to use 0.3moles or greater, preferably 0.5-50 moles in general, more
preferably 0.725 moles in particular.
[0074] The temperature condition of the dehydroxyfluorination of the
present invention is not particularly limited. It suffices to conduct it in a
range of-100 to +100°C, preferably -80 to +80°C in general, more preferably
-60 to +60°C in particular. In the case of conducting the reaction under a
temperature condition that is not lower than boiling point (-49.7°C) of

sulfuryl fluoride, it is possible to use a pressure-proof reaction vessel.
[0075] The pressure condition of the dehydroxyfluorination of the present
invention is not particularly limited. It suffices to conduct it in a range of
atmospheric pressure to 2MPa, preferably atmospheric pressure to 1.5MPa
in general, more preferably atmospheric pressure to 1MPa in particular.
Therefore, it is preferable to conduct the reaction using a pressure-proof
reaction vessel made of a material such as stainless steel (SUS) or glass
(glass lining).
[0076] The reaction time of the dehydroxyfluorination of the present
invention is not particularly limited. It suffices to conduct it in a range of
0.1 to 72 hours. Since it depends on substrate and the reaction conditions,
it is preferable to determine the time, at which the raw material has almost
disappeared, as the end point, while tracing the progress of the reaction by
an analytical means such as gas chromatography, liquid chromatography, or
NMR.
[0077] The post-treatrrfent of the dehydroxyfluorination of the present
invention is not particularly limited. Normally, it is possible to obtain a
crude product by pouring the reaction-terminated liquid into water or an
aqueous solution of inorganic base (for example, sodium hydrogencarbonate,
potassium hydrogencarbonate, sodium carbonate or potassium carbonate) of
alkali metal, followed by extraction with an organic solvent (for example,
toluene, mesitylene, methylene chloride or ethyl acetate). A salt formed of
fluorosulfuric acid and organic base or an alkali metal salt of fluorosulfuric
acid, which is produced as a by-product from sulfuryl fluoride, is remarkably
high in distribution to water. Therefore, it is possible to efficiently remove
these salts by an easy operation such as washing with water and to obtain
the target fluoro derivative with high chemical purity. According to need, it
can be purified to have a higher chemical purity by activated carbon
treatment, distillation, recrystallization and the like.
EXAMPLES
[0078] In the following, embodiments of the present invention are

specifically explained by examples. The present invention is, however, not
limited to these examples.
[0079] [EXAMPLE 1]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 2.45g (9.99mmol, 1.00eq) of 4-hydroxyproline derivative
represented by the following formula,
[Chemical Formula 19]

as a brown-color, oil-like substance. The recovered amount of the crude
product was slightly greater than the weight of the theoretical yield.
10.0mLof acetonitrile, and 1.10g (10.87mmol, 1.09eq) of triethylamine,
followed by lowering the inside temperature to -40°C and then bubbling
2.00g (I9.60mmol, 1.96eq) of sulfuryl fluoride from a cylinder. The inside
temperature was returned to room temperature, and stirring was conducted
for 20 hours and 20 minutes. Conversion of the reaction was found by gas
chromatography measurement to be 100%. The reaction-terminated liquid
was poured into a potassium carbonate aqueous solution [prepared from
2.80g (20.26mmol, 2.03eq) of potassium carbonate and 50.0mL of water],
followed by extraction two times with 50.0mL of ethyl acetate. The
recovered organic layer was concentrated under reduced pressure, followed
by vacuum drying, thereby obtaining a crude product of 4-fluoroproline
derivative represented by the following formula,
[Chemical Formula 20]

Selectivity of the crude product was found by gas chromatography
measurement to be 82.4% (As major three kinds of impurities were named
Impurities A-C, Impurity A, Impurity B and Impurity C were respectively
contained by 8.2%, 3.3% and 4.9%.) Instrument data of the crude product of
the obtained 4-fluoroproline derivative are shown in the following (assigned
as a mixture of E/Z isomers resulting from the NBoc group). It was found
by 19F-NMR spectrum that the crude product did not contain at all a salt
(FSO3H Et3N or FSO3K) derived from fluorosulfuric acid.
[0080] 1H-NMR (standard substance: Me4Si, heavy solvent: CDCl3), 5ppm:
1.43&1.49 (sx2, total 9H), 1.95-2.55 (total 2H), 3.51-3.94 (total 2H), 3.75 (S,
3H), 4.36-4.58 (total 1H), 5.10-5.31 (total 1H).
19F-NMR (standard substance: C6F6) heavy solvent: CDCl3), 5ppm: -11.27
(total 1F).
[0081] [EXAMPLE 2]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 2.45g (9.99mmol, l.OOeq) of 4-hydroxyproline derivative
represented by the following formula,
[Chemical Formula 21]

13.0mL of acetonitrile, 3.50g (34.59mmol, 3.46eq) of triethylamine, and 1.60g
(9.92mmol, 0.99eq) of triethylamine tris(hydrogen fluoride) complex,
followed by lowering the inside temperature to -40°C and then bubbling
2.00g (l9.60mmol, 1.96eq) of sulfuryl fluoride from a cylinder. The inside
temperature was returned to room temperature, and stirring was conducted
for 20 hours. Conversion of the reaction was found by gas chromatography
measurement to be 100%. The reaction-terminated liquid was poured into a
potassium carbonate aqueous solution [prepared from 6.30g (45.58mmol,

4.56eq) of potassium carbonate and 100.0mL of water], followed by
extraction two times with 100.0mL of ethyl acetate. The recovered organic
layer was concentrated under reduced pressure, followed by vacuum drying,
thereby obtaining a crude product of 4-fluoroproline derivative represented
by the following formula,
[Chemical Formula 22]

as a brown-color, oil-like substance. The recovered amount of the crude
product was slightly greater than the weight of the theoretical yield.
Selectivity of the crude product was found by gas chromatography
measurement to be 91.0% (As major three kinds of impurities were named
Impurities A-C, Impurity A, Impurity B and Impurity C were respectively
contained by 6.4%, 2.4% and 0.1%.) Instrument data of the crude product of
the obtained 4-fluoroproline derivative were similar to those of Example 1.
[0082] [EXAMPLE 3]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 12.30g (29.82mmol, 1.00eq) of 1-β-D-arabinofuranosyluracil
derivative represented by the following formula,
[Chemical Formula 23]

38.0mL of acetonitrile, 18.15g (l79.37mmol, 6.02eq) of triethylamine, and
19.30g (ll9.71mmol, 4.01eq) of triethylamine tris(hydrogen fluoride)
complex, followed by lowering the inside temperature to -40°C and then
bubbling lO.OOg (97.98mmol, 3.29eq) of sulfuryl fluoride from a cylinder.
The inside temperature was returned to room temperature, and stirring was
conducted for 16 hours and 30 minutes and then at 40°C for 5 hours and 30
minutes. Conversion of the reaction was found by liquid chromatography
measurement to be not lower than 99%. The reaction-terminated liquid
was poured into a potassium carbonate aqueous solution [prepared from
58.00g (419.65mmol, 14.07eq) of potassium carbonate and 300.0mL of water],
followed by extraction two times with 300.0mL of ethyl acetate. The
recovered organic layer was washed with 200.0mL of 10% brine, followed by
concentration under reduced pressure and vacuum drying, thereby obtaining
12.83g of a crude product of 2'-deoxy-2'-fluorouridine derivative represented
by the following formula,
[Chemical Formula 24]

as a brown-color, oil-like substance. The recovered amount of the crude
product was slightly greater than the weight of the theoretical yield.
Selectivity of the crude product was found by liquid chromatography
measurement to be 83.2%. Instrument data of the crude product of the
obtained 2'-deoxy-2'-fluorouridine derivative are shown in the following (four
kinds of diastereomers resulting from two THP groups were observed).
[0083] 19F-NMR (standard substance: C6F6, heavy solvent: CDC13), 5ppm:

-43.13 (dt, 51.9Hz, 15.4Hz), -42.50 (dt, 51.5Hz, 15.4Hz), -37.62 (dt, 51.5Hz,
15.0Hz), -37.55 (dt, 51.9Hz, 15.0Hz)/total 1F.
[0084] [EXAMPLE 4]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 9.60g (81.27mmol, l.OOeq, optical purity: 98.4%ee) of an
optically-active, orhydroxyearboxylate derivative represented by the
following formula,
[Chemical Formula 25]

Selectivity of the crude product was found by gas chromatography
27.0mL of mesitylene, and 8.50g (84.00mmol, 1.03eq) of trie thy lamine,
followed by lowering the inside temperature to -40°C and then bubbling
11.50 g (ll2.68mmol, 1.39eq) of sulfuryl fluoride from a cylinder. The
inside temperature was returned to room temperature, and stirring was
conducted for 22 hours and 10 minutes. Conversion of the reaction was
found by gas chromatography measurement to be 100%. The
reaction-terminated liquid was poured into a potassium carbonate aqueous
solution [prepared from 7.90g (57.16mmol, 0.70eq) of potassium carbonate
and 100.0mL of water], followed by extraction two times with 45.0mL of
mesitylene. The recovered organic layer was washed with a hydrochloric
acid brine (prepared from 95.0mL of 1N hydrochloric acid and 10.00g of
common salt), thereby obtaining 110.63g of a mesitylene solution of a crude
product of an optically-active, orfluorocarboxylate derivative represented by
the following formula.
[Chemical Formula 26]

measurement to be not less than 99.0% (except mesitylene). The
mesitylene solution of the crude product was subjected to a fractional
distillation (81-90°C/20000Pa), thereby recovering 26.82g of a main fraction.
The main fraction was found by 1H-NMR spectrum to contain 46.90mmol of
the optically-active, orfluorocarboxylate derivative, and the main fraction
concentration was 21.0wt%. The total yield was 58%. Optical purity and
instrument data of the main fraction of the obtained optically-active,
orfluorocarboxylate derivative are shown in the following.
[0085] Optical purity: 97.7%ee (It was determined by conducting a hydride
reduction using excessive aluminum lithium hydride in tetrahydrofuran,
then by leading the obtained (R)-2-fluoro-l-propanol into Mosher ester, and
then by conducting gas chromatography. Asymmetry transcription
percentage was 99.3%.)
[0086] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), 5ppm:
1.32 (t, 7.2Hz, 3H), 1.58 (dd, 23.6Hz, 6.9Hz, 3H), 4.26 (q, 7.2Hz, 2H), 5.00 (dq,
49.0Hz, 6.9Hz, 1H).
19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), 5ppm: -21.88 (dq,
48.9Hz, 24.4Hz, 1F)
[0087] [EXAMPLE 5]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 3.50g (l5.00mmol, l.OOeq) of a primary alcohol derivative
represented by the following formula,
[Chemical Formula 27]

30.0mLof acetonitrile, 8.35g (82.52mmol, 5.50eq) of triethylamine, and 4.84g
(30.02mmol, 2.00eq) of triethylamine tris(hydrogen fluoride) complex,
followed by lowering the inside temperature to -40°C and then bubbling

7.86g (77.01mmol, 5.13eq) of sulfuryl fluoride from a cylinder. The inside
temperature was returned to room temperature, and stirring was conducted
for 1 hr and 10 minutes. Stirring was further conducted at 60°C for 39
hours and 30 minutes. Conversion of the reaction was found by gas
chromatography measurement to be 100%. 50.0mL of water were added to
the reaction-terminated liquid, followed by concentration under reduced
pressure, then adding 50.0mL of water to the concentrated residue, and then
conducting an extraction one time with lOO.OmL of ethyl acetate. The
recovered organic layer was dried with anhydrous sodium sulfate, followed
by concentration under reduced pressure and vacuum drying, thereby
obtaining 2.72g of a crude product of a monofluoromethyl derivative
represented by the following formula,
[Chemical Formula 28]

as a dark brown color, oil-like substance. Selectivity of the crude product
was found by gas chromatography measurement to be 69.4%. The crude
product was found by internal standard method (internal standard
substance: C6F6) of 19F-NMR to contain 3.45mmol of the monofluoromethyl
derivative. The yield was 23%. Instrument data of the crude product of
the obtained monofluoromethyl derivative are shown in the following.
[0088] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), 5ppm:
0.90 (d, 6.8Hz, 3H), 1.08 (d, 6.8Hz, 3H), 2.44 (m, 1H), 4.24 (m, 1H), 4.76 (ddd,
46.6Hz, 9.5Hz, 4.8Hz, 1H), 5.01 (dt, 46.6Hz, 9.5Hz, 1H), 7.74 (Ar-H, 2H), 7.86
(Ar-H, 2H).
19F-NMR (standard substance-: C6F6, heavy solvent: CDCl3), δppm: -62.12 (dt,
13.3Hz, 46.6Hz, 1F).
[0089] It is possible to produce the primary alcohol derivative of the raw

material substrate from a commercial optically active valinol by referring to
Protective Groups in Organic Synthesis, Third Edition, 1999, John Wiley &
Sons, Inc. The obtained monofluoromethyl derivative can be converted to
optically active l-isopropyl-2-fluoroethylamine without damaging optical
purity by referring to the same book.
[0090] [EXAMPLE 6]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 1.39g (7.98mmol, l.OOeq) of a primary alcohol derivative
represented by the following formula,
[Chemical Formula 29]

as a brown color, oil-like substance. Selectivity of the crude product was
found by gas chromatography measurement to be 98.6%. The yield was
16.0mL of acetonitrile, 4.45g (43.98mmol, 5.51eq) of triethylamine, and 2.58g
(16.00mmol, 2.01eq) of triethylamine tris(hydrogen fluoride) complex,
followed by lowering the inside temperature to -40°C and then bubbling
3.00g (29.39mmol, 3.68eq) of sulfuryl fluoride from a cylinder. The inside
temperature was returned to room temperature, and stirring was conducted
for 19 hr and 15 minutes. Conversion of the reaction was found by gas
chromatography measurement to be 100%. 10.0mL of water were added to
the reaction-terminated liquid, followed by concentrating acetonitrile under
reduced pressure and then conducting an extraction of the concentrated
residue one time with 30.0mL of ethyl acetate. The recovered organic layer
was washed with 10.0mL of saturated brine, followed by drying with
anhydrous sodium sulfate, concentration under reduced pressure and
vacuum drying, thereby obtaining 0.36g of a crude product of a
monofluoromethyl derivative represented by the following formula,
[Chemical Formula 30]

26%. Instrument data of the crude product of the obtained
monofluoromethyl derivative are shown in the following.
[0091] 1H-NMR (standard substance-' Me4Si, heavy solvent: CDCl3), δppm:
1.42-1.88 (m, 10H), 3.35-3.52 (m, 2H), 3.70-3.88 (m, 2H), 4.45 (dt, 46.8Hz,
6.1Hz, 2H), 4.56 (m, 1H).
19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), δppm: -56.37
(septet, 23.4Hz, 1F).
[0092] It is possible to produce the primary alcohol derivative of the raw
material substrate from a commercial optically active 1,4-butanediol by
referring to Protective Groups in Organic Synthesis, Third Edition, 1999,
John Wiley & Sons, Inc. The obtained monofluoromethyl derivative can be
converted to 4-fluoro-1-butanol by referring to the same book.
[0093] [EXAMPLE 7]
A pressure-proof reaction vessel made of stainless steel (SUS) was
charged with 1.58g (9.98mmol, l.OOeq) of a primary alcohol derivative
represented by the following formula,
[Chemical Formula 31]

20.0mLof acetonitrile, 5.57g (55.04mmol, 5.52eq) of triethylamine, and 3.22g
(l9.97mmol, 2.00eq) of triethylamine tris(hydrogen fluoride) complex,
followed by lowering the inside temperature to -40°C and then bubbling
2.04g (l9.99mmol, 2.00eq) of sulfuryl fluoride from a cylinder. The inside
temperature was returned to room temperature, and stirring was conducted
for 22 hr and 20 minutes. Conversion of the reaction was found by gas
chromatography measurement to be 100%. 20.0mL of water were added to
the reaction-terminated liquid, followed by conducting an extraction one
time with 20.0mL of ethyl acetate. The recovered organic layer was washed
with 20.0mL of water and then with 20.0mL of saturated brine, followed by
drying with anhydrous sodium sulfate and concentration under reduced
pressure, thereby obtaining a crude product of a monofluoromethyl

derivative represented by the following formula,
[Chemical Formula 32]

as a brown color, oil-like substance. Selectivity of the crude product was
found by gas chromatography measurement to be 94.2%. The crude product
was found by internal standard method (internal standard substance: C6F6)
of 19F-NMR to contain 2.10mmol of the monofluoromethyl derivative. The
yield was 21%. Instrument data of the crude product of the obtained
monofluoromethyl derivative are shown in the following.
[0094] 1H-NMR (standard substance: Me4Si, heavy solvent: CDC13), δppm:
0.89 (t, 6.8Hz, 3H), 1.20-1.45 (m, 14H), 1.60-1.70 (m, 2H), 4.44 (dt, 47.6Hz,
6.2Hz, 2H).
19F-NMR (standard substance: C6F6, heavy solvent: CDCl3), 5ppm: -55.97
(septet, 23.8Hz, 1F).
[0095] A commercial product was used as the primary alcohol derivative of
the raw material substrate.

WE CLAIM:
1. A dehydroxyfluorination agent comprising:
sulfuryl fluoride (SO2F2); and
an organic base that is free from a free hydroxyl group in the molecule.
2. A dehydroxyfluorination agent according to claim 1, wherein a ratio of the
sulfuryl fluoride by mol number to the organic base is in a range of 1:5 to 5:1.
3. A dehydroxyfluorination agent according to claim 1 or claim 2, further
comprising a hydrogen fluoride source added from outside of system, the hydrogen
fluoride source being defined as hydrogen fluoride or a salt or complex formed
between hydrogen fluoride and an organic base.
4. A dehydroxyfluorination agent according to claim 3, wherein a ratio of the
sulfuryl fluoride by mol number to the hydrogen fluoride source (in terms of HF)
added from the outside of the system is in a range of 1:10 to 3;1.
5. A dehydroxyfluorination agent according to any one of claim 1 to claim 4,
wherein the organic base is selected from the group consisting of trimethylamine,
triethylamine, diisopropylethylamine, tri-n-propylamine, pyridine, 2,3-lutidine, 2,4-
lutidine, 2,5-lutidine, 2,6-lutidine, 3,4-lutidine, 3,5-lutidine, 2,3,4-collidine, 2,4,5-
collidine, 2,5,6-collidine, 2,4,6-collidine, 3,4,5-collidine, and 3,5,6-collidine.
6. A dehydroxyfluorination agent according to any one of claim 1 to claim 5,
further comprising an aprotic organic solvent.

There is provided a novel, useful dehydroxyfluorination agent
containing sulfuryl fluoride (SO2F2) and an organic base that is free from a
free hydroxyl group in the molecule. According to the present
dehydroxyfluorination agent, it is not necessary to use
perfluoroalkanesulfonyl fluoride, which is not preferable in large-scale use,
and it is possible to advantageously produce optically-active fluoro
derivatives, which are important intermediates of medicines, agricultural
chemicals and optical materials, for example, 4-fluoroproline derivatives,
2'-deoxy-2'-fluorouridine derivatives, optically-active α-fluorocarboxylate
derivatives, and monofluoromethyl derivatives, even in large scale.

Documents:

4637-KOLNP-2008-(14-12-2012)-AMANDED PAGES OF SPECIFICATION.pdf

4637-KOLNP-2008-(14-12-2012)-ANNEXURE TO FORM 3.pdf

4637-KOLNP-2008-(14-12-2012)-CLAIMS.pdf

4637-KOLNP-2008-(14-12-2012)-CORRESPONDENCE.pdf

4637-KOLNP-2008-(14-12-2012)-OTHERS.pdf

4637-KOLNP-2008-(14-12-2012)-PETITION UNDER RULE 137-1.pdf

4637-KOLNP-2008-(14-12-2012)-PETITION UNDER RULE 137.pdf

4637-KOLNP-2008-(28-10-2014)-CLAIMS.pdf

4637-kolnp-2008-abstract.pdf

4637-kolnp-2008-claims.pdf

4637-kolnp-2008-correspondence.pdf

4637-kolnp-2008-description (complete).pdf

4637-kolnp-2008-form 1.pdf

4637-kolnp-2008-form 18.pdf

4637-kolnp-2008-form 2.pdf

4637-kolnp-2008-form 3.pdf

4637-kolnp-2008-form 5.pdf

4637-kolnp-2008-international publication.pdf

4637-kolnp-2008-international search report.pdf

4637-kolnp-2008-specification.pdf

4637-kolnp-2008-translated copy of priority document.pdf

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Patent Number

263454

Indian Patent Application Number

4637/KOLNP/2008

PG Journal Number

44/2014

Publication Date

31-Oct-2014

Grant Date

29-Oct-2014

Date of Filing

17-Nov-2008

Name of Patentee

CENTRAL GLASS COMPANY, LIMITED

Applicant Address

5253, OAZA OKIUBE, UBE-SHI, YAMAGUCHI

Inventors:

#	Inventor's Name	Inventor's Address
1	TAKASHI OOTSUKA	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
2	AKIHIRO ISHII	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
3	MANABU YASUMOTO	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
4	HIDEYUKI TSURUTA	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
5	KENJIN INOMIYA	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
6	KOJI UEDA	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151
7	KAORI MOGI	C/O CHEMICAL RESEARCH CENTER OF CENTRAL GLASS COMPANY, LIMITED, 2805 IMAFUKUNAKADAI, KAWAGOE-SHI, SAITAMA 350-1151

PCT International Classification Number

C07B 55/00

PCT International Application Number

PCT/JP2007/062687

PCT International Filing date

2007-06-25

PCT Conventions:

#	PCT Application Number	Date of Convention	Priority Country
1	2006-182235	2006-06-30	Japan