| Title of Invention | "A NOVEL BENZYL CARBAMATES" |
|---|---|
| Abstract | Compounds according to general formula (1), wherein G1 is NR5R6 or a fused polycyclic group are novel. They are selective and potent oxytocin agonists. Pharmaceutical compositions of such compounds are useful in the treatment of, inter alia, erectile dysfunction. |
| Full Text | FIELD OF THE INVENTION The present invention relates to a series of non-peptide oxytocin agonists and to pharmaceutical compositions comprising such compounds. The compositions are useful for the treatment of certain physiological disorders, such as erectile dysfunction. BACKGROUND Neurophvseal hormones The neurophyseal hormones oxytocin (OT) and vasopressin (VP) are cyclic nonapeptides secreted by the posterior pituitary gland. The structure of oxytocin is shown below. (Formula Removed) Vasopressin differs from oxytocin in that it has phenylalanine at position 3 in place of isoleucine and arginine at position 8 in place of leucine. Both hormones are synthesised in vivo as larger precursors, neurophysins, which are subject to post-translational processing to release the mature peptides. OT and VP act through a family of heptahelical receptors. The first target organs to be identified for OT were the uterus, where it is implicated in the onset and progress of labour, and mammary glands, where it is involved in the regulation of milk expression. Other organs also express OT receptors, and it is clear that OT has a range of physiological roles that have not been fully elaborated yet. In particular, it has been suggested that OT acting in the CNS is involved in the erectile response in males, and in the regulation of female sexual arousal. For example, OT is erectogenic when administered i.c.v. to male rats. It also has erectogenic activity when given i.v., but the doses required are up to two orders of magnitude greater, which is consistent with a central mode of action. Oxvtocin agonists and antagonists A number of peptide analogues of OT are known in the literature. These include both agonists and antagonists. OT and its agonists are used, for example, to accelerate labour and to increase uterine muscle tone to control post-partum bleeding, and one antagonist, atosiban, has recently been registered as a treatment for pre-term labour. However, the peptidic nature of these compounds means that they are not likely to be bioavailable after oral dosing or to cross efficiently into the CNS. In order to get drugs that can be given orally and to be able to exploit the central effects of OT, attention has increasingly turned to non-peptides. As a result, there are many publications describing non-peptide OT antagonists in early-stage development. So far, however, there have been no reports of non-peptide OT agonists. This is not unexpected, as it is generally held that it is easier to find a receptor antagonist than an agonist. So there remains a need for non-peptide OT receptor agonists. Such compounds should preferably be selective for the OT receptor over the VP receptors. They could be expected to show therapeutic utility in male and female sexual dysfunction, particularly male erectile dysfunction, in promoting labour, in controlling post-partum bleeding, in increasing milk let-down as well as a number of other indications. SUMMARY OF THE INVENTION We describe herein a series of potent and specific OT receptor agonists. In a first aspect, the present invention comprises novel compounds according to general formula 1 , and pharmaceutically acceptable salts thereof. (Figure Removed) G1 is a group according to general formula 2, 3, 4, 5, 6 or 7. (Figure Removed) A1 is CH2, CH(OH), NH, N-alkyl, O or S; A2 is CH2) CH(OH), C(=O) or NH; A3 is S, NH, N-alkyl, -CH=CH- or -CH=N-; A4 and A5 are each CH or N; A6 is CH2l NH, N-alkyl or O; A7 and A11 are C or N; A8 and A9 are CH, N, NH, N(CH2)dR7 or S; A10 is -CH=CH-, CH, N, NH, N-(CH2)d-R7 or S; A12 and A13 are N or C and A14, A15 and A16 are NH. N-CH3, S, N or CH, provided that not more than one of A8, A9 and A10 is NH, N-(CH2)d-R7 or S; that A7 and A11 are not both simultaneously N; that neither A7 nor A11 is N if one of A8, A9 and A10 is NH, N-(CH2)d-R7 or S; that if A10 is -CH=CH- then A8 is N, A9 is CH and both A7 and A11 are C; that if A10 is not -CH=CH- then one of A8, A9 and A10 is NH, N-(CH2)d-R7 or S or one of A7 and A11 is N; that not more than one of A14, A15 and A16 is NH, N-CH3 or S; that A12 and A13 are not both simultaneously N; that if one of A14, A15 and A16 is NH, N-CH3 or S then A12 and A13 are both C; and that one of A14, A15 and A16 is NH, N-CH3 or S or one of A12 and A13 is N. X1 is O or NH. R1, R2 and R3 are each H, alkyl, O-alkyl, F, Cl or Br. R4 is H, alkyl, optionally substituted phenyl, pyridyl, thienyl or furyl, or is -(CH2)e-R8. Rs and R6 are each independently alkyl, Ar or -(CH2)rAr, where Ar is optionally substituted phenyl or thienyl. R7 and R8 are each independently H, alkyl, optionally substituted phenyl, pyridyl, thienyl or furyl, F, OH, O-alkyl, S-alkyl, O-acyl, NH2, NH-alkyl, N(alkyl)2, NH-acyl, N(alkyl)-acyl, C02H, CO2-alkyl, CONH2, CONH-alkyl, CON(alkyl)2, CN or CF3. a is 1 or 2, b is 1, 2 or 3, c is 1 or 2, d is 1, 2 or 3; e is 1, 2 or 3 and f is 1, 2 or 3. In a second aspect, the present invention comprises pharmaceutical compositions of these novel compounds, which compositions are useful for the treatment of, inter alia, male erectile dysfunction. In further aspects, the present invention comprises the use of such compositions in therapy and therapeutic methods using the compositions. DETAILED DESCRIPTION OF THE INVENTION In a first aspect, the present invention comprises novel benzyl carbamates and ureas according to general formula 1. (Figure Removed) In this general formula the substituents R1, R2 and R3 are independently selected from hydrogen (H), alkyl groups, alkoxy (O-alkyl) groups, and the halogens fluorine (F), chlorine (Cl) and bromine (Br). Preferably, at least one of R1, R2 and R3 is H and at least one is not H. More preferably, one of R1, R2 and R3 is an alkyl group or a halogen and the others are H. Most preferably, R1 is methyl or Cl and R2 and R3 are both H. The linking group X1 is selected from oxygen (O) and unsubstituted nitrogen (NH). Preferably, X1 is NH. The integer a may be 1 or 2, and the integer b may be 1, 2 or 3. Preferably a is 1 and b is 2 such that this ring is a piperazine. The substituent R4 is selected from H, alkyl groups, optionally substituted phenyl, pyridyl, thienyl, furyl, pyrrolyl, pyrazolyl, imidazolyl, oxazolyl, isoxazolyl, thiazolyl and isothiazolyl groups, a group-(CO)-O-(CH2)eR8 where e is 1, 2, 3 or 4, a group -(CH2)eR8, where e is 1, 2, 3 or 4, -CH2-CH=CH-CH2-R8, -CH2-CsC-CH2-R8, -(CH2)g-CH(OH)-(CH2)h-R8, where g and h are independently 1 or 2, ~(CH2)rO-(CH2)rR8 where i and j are independently 1 or 2,and CHj ^—-*—R8 R8 is selected from H, F, CF3l alkyl groups, O-alkyl groups, S-alkyl groups, O-acyl groups, hydroxyalkyl groups, amino groups such as NH2, NH-alkyl, N(alkyl)2l 1-pyrrolidinyl, 1-piperidinyl and 4-morpholinyl, NH-acyl, N(alkyl)-acyl, CO2H, CCValkyl, CONH2( CONH-alkyl, CON(alkyl)2, CN and optionally substituted phenyl, pyridyl, thienyl, furyl, pyrrolyl, pyrazolyl, imidazolyl, oxazolyl, isoxazolyl, thiazolyl and isothiazolyl groups. Suitable optional substituents for the phenyl, pyridyl, thienyl, furyl, pyrrolyl, pyrazolyl, imidazolyl, oxazolyl, isoxazolyl, thiazolyl and isothiazolyl groups in R4 and R8 include F, Cl, Br, CF3, alkyl groups, OH, O-aikyl groups, hydroxyalkyl groups, amino groups such as NH2, NH-alkyl and N(alkyl)2, NH-acyl, N(alkyl)-acyl, CO2H, CO2-alkyl, CONH2, CONH-alkyl, CON(alkyl)2, oxadiazolyl, thiadiazolyl, CN and NO2. The phenyl, pyridyl, thienyl furyl, pyrrolyl, pyrazolyl, imidazolyl, oxazolyl, isoxazqlyl, thiazolyl or isothiazolyl group may have up to three such substituents which may be the same or different. The group G1 is a disubstituted nitrogen such that the C(=O)-G1 bond is an amide bond. G1 is selected from an acyclic group according to general formula 2, a fused bicyclic group according to general formulae 3, 4 and 5, and a fused tricyclic group according to general formulae 6 and 7, (Figure Removed) In general formula 2, R5 and R6 are independently selected from alkyl, Ar and -(CH2)r-Ar, where f is 1, 2 or 3 and Ar is selected from thienyl and optionally substituted phenyl. Suitable substituents for the phenyl group are alkyl groups, OH, alkoxy groups, halogens, NH2, NH-alkyl and N(alkyl)2. The phenyl group may be substituted with up to three such substituents which may be the same or different. In general formula 3, A1 is selected from CH2, CH(OH), NH, N-alkyl, O and S. A2 is selected from CH2, CH(OH), C(=O) and NH, and c is 1 or 2, preferably 2. It is preferred that when A2 is NH then A1 is CH2. It is also preferred that when A2 is C(=O) then A1 is NH or N-alkyl. In general formulae 3, 6 and 7, A3 is selected from S, NH, N-alkyl, -CH=CH- and -CH=N- and A4 and A5 are each selected from CH and N. In a preferred embodiment, A3 is S and A4 and A5 are both CH, so as to form a thiophene ring. In another preferred embodiment, A3 is -CH=CH- and A4 and A5 are both CH, so as to form a benzene ring. In another preferred embodiment, A3 is -CH=N- and A4 and A5 are both CH, so as to form a pyridine ring. In another preferred embodiment, A3 is -CH=CH-, A4 is CH and A5 is N, again so as to form a pyridine ring. In general formulae 4 and 6, A6 is selected from CH2, NH, N-alkyl and O, A7 and A11 are selected from C and N, A8 and A9 are selected from CH, N, NH, N-(CH2)d-R7 and S and A10 is selected from -CH=CH-, CH, N, NH, N-(CH2)d-R7 and S, where d is 1, 2 or 3 and R7 is selected from H, F, CF3, alkyl groups, OH, O-alkyl groups, S-alkyl groups, O-acyl groups, amino groups such as NH2, NH-alkyl and N(alkyl)2l NH-acyl, N(alkyl)-acyl, CO2H, COz-alkyl, CONH2, CONH-alkyl, CON(alkyl)2, CN and optionally substituted phenyl groups. Suitable optional substituents for the phenyl groups in R7 include F, Ci, Br, CF3, alkyl groups, O-alkyl groups, amino groups such as NH2, NH-alkyl and N(alkyl)2, NH-acyl, N(alkyl)-acyl, CO2H, CO2-alkyl, CONH2, CONH-alkyl, CON(alkyl)2, CN and NO2. The phenyl group may have up to three such substituents which may be the same or different. The ring constituted by A7, A8, A9, A10 and A11 is aromatic, and accordingly the groups must satisfy certain requirements. When A10 is -CH=CH- the ring is a six-membered ring. As such, it can only comprise atoms of the type -C(R)= and -N=. Hence A7 and A11 must both be C and A8 and A9 must be either CH or N. We have found that suitable activity is only obtained when A8 is N and A9 is CH. When A10 is not -CH=CH- then the ring is a five-membered ring. In this case one, and only one, of the atoms in the ring must be S or a trigonal nitrogen. In this context, a "trigonal nitrogen" is a nitrogen atom linked covalently to three different atoms. Two of these atoms are the immediate neighbours to the nitrogen atom in the five-membered ring. The third is a hydrogen, carbon or other atom linked to the five-membered ring. Thus it follows that, when A10 is not -CH=CH- then one (and only one) of A7, A8, A9, A10 and A11 must be S or a trigonal nitrogen. Hence the selection of A7, AB, AB, A10 and A11 is subject to the following restrictions. 1) If A10 is not -CH=CH- then one of A8, A9 and A10 is NH, N-(CH2)d-R7 or S or one of A7 and A11 is N. 2) Not more than one of A8, A9 and A10 may be NH, N-(CH2)d-R7 or S. 3) A7 and A11 may not both simultaneously be N. 4) Neither A7 nor A11 may be N if one of A8, A9 and A10 is NH, N(CH2)dR7 or S. In a preferred embodiment, A6 is NH. In another preferred embodiment, A8 is NH or N-(CH2) 1) One of A14, A15 and A16 is NH, N-CH3 or S or one of A12 and A13 is N. 2) Not more than one of A14, A15 and A16 is NH, N-CH3 or S. 3) A12 and A13 may not both simultaneously be N. 4) If one of A14, A15 and A16 is NH, N-CH3 or S then A12 and A13 are both C As used herein, the term "alky!" is intended to designate lower alkyl groups, i.e. saturated hydrocarbon groups of between one and six carbon atoms, including linear, branched and cyclic alkyl groups. Examples of "alkyl" include, but are not limited to: C^ - methyl, C2 - ethyl, C3 - propyl, isopropyl, cyclopropyl, C4 - n-butyl, sec-butyl, isobutyl, tert-butyl, cyclobutyl, cyclopropylmethyl, methylcyclopropyl, C5 - n-pentyl, neopentyl, cyclopropylethyl, dimethylcyclopropyl, and C6-n-hexyl, cyclohexyl, bicyclo[3.1.0]hexyl. The term "alkenyl" denotes a lower alkenyl group, i.e. a mono-unsaturated hydrocarbon group of between two and six carbon atoms, including linear, branched and cyclic alkenyl groups. Examples of "alkenyP include, but are not limited to: C2 - vinyl, C3 - allyl, 1-methylvinyl, 1-propenyl, C4 - but-3-enyl, but-2-enyl, methallyl. The term "alkynyl" denotes a lower alkynyl group, i.e. an unsaturated hydrocarbon group of between two and six carbon atoms which includes a carbon-carbon triple bond, including linear, branched and cyclic alkynyl groups. Examples of "alkynyl" include, but are not limited to: C2 - ethynyl, C3 - propargyl, 1-propynyl. The term "hydroxyalkyl" denotes an alkyl group as defined above in which one or more of the hydrogen atoms are replaced by hydroxyl groups (OH). In general, not more than one hydroxyl group will be attached to any particular carbon atom within the hydroxalkyl group. Examples of hydroxyalkyl groups include, but are not limited to: hydroxymethyl (HOCH2), 1-hydroxyethyi (CH3CH(OH)), 2-hydroxyethyl (HOCH2CH2), 1,2-dihydroxyethyl (HOCH2CH(OH)) 4-hydroxy-2-pentyl (CH3CH The compounds according to the present invention generally contain a basic nitrogen atom and so are capable of forming addition salts with protic acids such as hydrochloric acid, sulphuric acid, phosphoric acid, acetic acid, trifluoroacetic acid, benzoic acid, maleic acid, citric acid, fumaric acid, methanesulphonic acid and the like. The compounds of the present invention may also contain an acidic group, such as a carboxylic acid group at R7 or R8 These compounds may exist as inner salts (zwitterions) or as salts such as sodium, potassium, magnesium, calcium or tetra-alkylammonium salts. To the extent that such salts are pharmaceutically acceptable, they are included within the scope of the present invention. The compounds according to the present invention may have one or more stereogenic centres ("asymmetric carbon atoms") and so may exhibit optical isomerism. The scope of the present invention includes all epimers, enantiomers and diastereomers of compounds according to general formula 1, including single isomers, mixtures and racemates. Particularly preferred embodiments within the present invention are those compounds that combine two or more of the preferred features described above. One such particularly preferred embodiment is a urea according to general formula 8. (Figure Removed) In general formula 8, R1A is methyl or Cl. G1, R4, a and b are as previously defined. More preferred is a urea according to general formula 9. (Figure Removed) 9 In general formula 9, R1A, R4 and G1 are as previously defined. Another particularly preferred embodiment is a compound according to general formula 10, which corresponds to a compound according to general formula 1 in which G1 is a group according to general formula 6 wherein A4, A5and A10 are all CH, A6 is NH, A7 and A11 are both C, A8 is N(CH2)dR7 and A9 is N. (Figure Removed) In general formula 10, R1, R2, R3, R4, R7, A3, X1, a, b and d are as previously defined. A most preferred embodiment is a compound according to general formula 11. (Figure Removed) In general formula 11, R , R , R7, A and d are as previously defined. Individual preferred compounds within the invention include: 5-(4-(4-cyclopropylmethylpiperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine, 5-(4-(4-benzylpiperazine-1 -carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-jb][1,5]benzodiazepine, 5-(4-(4-(3-hydroxybenzyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-jb][1,5]benzodiazepine, 5-(4-(4_(3-hydroxymethylbenzyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-f)][1,5]benzodiazepine, 1 -methyl-5-(3-methyl-4-(4-(4-picolyl)piperazine-1 -carbonylaminomethyl)benzoyl)-4,10-dihydropyrazolo[5,4-d][1,5]benzodiazepine, 5-(4-(4-(2-hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-/3][1,5]benzodiazepine, 1-methyl-5-(3-methyl-4-(4-(3-(methylthio)propyl)piperazine-1-carbonylaminomethyl)benzoyl)-4,10-dihydropyra2olo[5,4-Jb][1,5]benzodiazepine, 5-(4-(4-(2-aminoethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-jb][1,5]benzodiazepine, and 5-(4-(4-(2-hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-/)][1,4]diazepine. The compounds of the present invention can be prepared by standard chemical manipulations. In general, compounds according to general formula 1 can be considered to consist of three component parts: • Component C1 corresponding to G1 • Component C2 corresponding to the substituted benzoyl unit • Component C3 corresponding to the saturated heterocycle (Figure Removed) Intermediates corresponding to these components are prepared and then assembled to give the final product. These three components are: for C1, a secondary amine(Figure Removed) It will be recognised that the substituted benzoic acid that serves for C2 has two functional groups, one of which will need temporary protection during the assembly of the final compound. The principles of functional group protection are well known in the art and are described in, for example, J.F.W. McOmie, "Protective Groups in Organic Chemistry", Plenum Press, 1973; T.W. Greene and P.G.M. Wuts, "Protective Groups in Organic Synthesis", 2nd edition, John Wiley, 1991; and P.J. Kocienski, "Protecting groups", Georg Thieme Verlag, 1994. The carboxylic acid group will usually be protected as an ester, such as the methyl, benzyl or tert-butyl ester. The primary amine of the benzoic acid (when X1 = NH) will usually be protected as a carbamate derivative such as the terf-butyl carbamate (BOC derivative), the benzyl carbamate (CBZ or more simply Z derivative) or the 9-fluorenylmethyl carbamate (Fmoc derivative). When X1 = O the resulting alcohol function will usually be protected as an ester such as an acetate, or an ether such as a methoxymethyl, tetrahydropyranyl or trialkylsilyl ether. Other functional groups may require protection. For example, the group G1 may include one or more primary or secondary amino groups which may need protection. In the following general description of the synthetic methodology it will be assumed that such protection is used when necessary. (i) Preparation of secondary amine for C1 Acyclic secondary amines corresponding to HNRSR5 are well known. Many are items of commerce. Those that are not may be prepared according to published methods or by simple modification of such methods. Some particularly useful methods are listed below, a) Alkylation (This method is only applicable in cases where further alkylation can be avoided.) b) Reductive amination (Figure Removed) Secondary amines corresponding to C1 where G11 is a group according to general formulae 3-7 are generally not commercially available. They can be prepared according to published methods, or by obvious modifications of such methods. Particularly useful methods are described in: Aranapakam et a/., Bioorg. Med. Chem. Lett. 1993, 1733; Artico et a/., Farmaco. Ed. Sci. 24, 1969, 276; Artico et a/., Farmaco. Ed. Sci. 32, 1977, 339; Chakrabarti et a/., J. Med. Chem. 23, 1980, 878; Chakrabarti et a/., J. Med. Chem. 23, 1980, 884; Chakrabarti ef a/., J. Med. Chem. 32, 1989, 2573; Chimirri ef a/., Heterocycles 36, 1993, 601; Grunewald et a/., J. Med. Chem. 39, 1996, 3539; Klunder ef a/., J. Med. Chem. 35, 1992, 1887; Liegeois ef a/., J. Med. Chem. 37, 1994, 519; Olagbemiro ef a/., J. Het. Chem. 19, 1982, 1501; Wright ef a/., J. Med. Chem. 23, 1980, 462; Yamamoto et ai, Tet. Lett. 24, 1983, 4711; and International patent application, publication number WO99/06403. (ii) Preparation of substituted benzole acid for C2 Substituted benzoic acids corresponding to C2 are not generally items of commerce, but they can be prepared using published methods or obvious variations of such methods. The main challenge is generally the elaboration of the -CH2X1H functionality at the 4-position. Some useful transformations are listed below, a) Bromination/Substitution (Figure Removed) ////') Preparation of heterocvcle derivative for C3 Certain heterocycles corresponding to C3, particularly A/-aryl piperazines, are items of commerce. Other heterocycles can be prepared according to the methods described in the literature. Useful transformations include the following. a) Alkylation or reductive alkylation RACH2CI Or /"((a NH ( ) RACHO / NaBH3CN (where PG is a protecting group and RACH2 is R4) b) Acylation/reduction /- 1.RACOCI >_ 2. LiAIH4 c) Reduction PG- R^ LiA,H4 With the three components, suitably protected if necessary, in hand, the assembly of the final compound requires the formation of two bonds: between C1 and C2, and between C2 and C3. These bond-forming steps may be taken in either order. Thus, the following sequences can be proposed: C1 + C2 -» C1C2 -> C1C2C3 C2 + C3 -» C2C3 -» C1C2C3 (i) Formation of Cf-C2 bond The bond between C1 and C2 is a simple amide bond. The chemistry for making such bonds from a carboxylic acid and a secondary amine is well known in the art of organic synthesis, and particularly in the field of peptide synthesis. The carboxylic acid may be converted into a more reactive species such as an acid chloride (using, for example oxalyl chloride or thionyl chloride) or a mixed anhydride (using isobutyl chloroformate). This reactive species is then added to the secondary amine in a suitable solvent, generally an aprotic solvent such as dichloromethane or dimethylformamide, in the presence of a base such as triethylamine or 4-dimethylaminopyridine, and the reaction is allowed to proceed at a temperature between -20°C and the boiling point of the solvent. The choice of temperature and the time allowed for the reaction will depend on the reactivity of the two components. Alternatively, the carboxylic acid and the secondary amine may be mixed in a suitable solvent as above, optionally in the presence of a base, and a condensing agent added. Suitable condensing agents include carbodiimides, such as dicyclohexylcarbodiimide (DCC) and N-ethyl-N'-dimethylaminopropylcarbodiimide (EDC, also WSCD for water-soluble carbodiimide), phosphorus reagents such as (benzotriazol-1-yloxy)-tris(dimethylamino)phosphonium hexafluorophosphate (BOP), (benzotriazol-1-yloxy)-tripyrrolidinophosphonium hexafluorophosphate (PyBOP®) and bromotripyrrolidino-phosphonium hexafluorophosphate (PyBroP®), and ureas such as O-(benzotriazoM-yl)-. N,N,N',N'-tetramethyIuronium hexafluorophosphate (HBTU). (/'/'} Formation of C^C3 bond The bond between C2 and C3 is a carbamate (when X1 = O) or a urea (when X1 = NH). The first step in the formation of this bond is generally to react the heterocycle derivative with phosgene or a phosgene equivalent such as trichloromethyl chloroformate, bis(trichloromethyl)carbonate or carbonyldiimidazole. Again, an aprotic solvent and a tertiary amine base will generally be used. The intermediate formed in this step is usually not isolated. The alcohol (X1 = O) or amine (X1 = NH) is added and the reaction is allowed to continue, directly forming the carbamate or urea. As an alternative, when X1 = NH the reactive intermediate may be formed by the reaction of C2 with the phosgene equivalent and the amine added in the second part of the synthesis. The compounds according to the present invention are useful in human and animal therapy. When so used, they will generally be formulated in an appropriate manner. Thus a second aspect of the present invention is a pharmaceutical formulation that includes a compound as described above as an active ingredient. A third aspect of the present invention is the use of a compound according to the first aspect in the manufacture of such a composition. The composition according to the present invention may be presented in any form that is known in the art. For example, the formulation may be presented as a tablet, capsule, powder, suppository, cream, solution or suspension, or in a more complex form such as an adhesive patch. The formulation will generally include one or more excipients, such as diluents, bulking agents, binding agents, dispersants, solvents, preservatives, flavoring agents and the like. Where the formulation is presented as a tablet or capsule the excipients may optionally include one or more agents to control the release of the active species, such as a coating of a polymer that is insoluble at low pH but soluble at neutral or high pH. Such a coating (known as an "enteric coating") prevents the release of the active agent in the stomach but allows its release in the intestines. The formulation may also include one or more additional pharmacologically active species. Preferably the formulation includes no such additional active agents. In further aspects, the present invention comprises the use of such compositions, and hence of the compounds of the invention, in human and animal therapy, and methods of treatment involving such use of the compositions and compounds. The compounds of the present invention are potent and selective oxytocin receptor agonists, and so the compositions are useful in the treatment of conditions for which inadequate oxytocin-like activity is implicated in the pathophysiology. Such conditions include, but are not limited to: sexual disorders such as male erectile dysfunction, ejaculatory disorders and female sexual dysfunction, cancer of the prostate, breast, ovary and bones, osteoporosis, benign prostatic hyperplasia, post-partum bleeding, and depression. The compositions may * also be used to induce labour or delivery of the placenta, to decrease arterial blood pressure, to decrease exaggerated responses to stress and to increase the nociceptive threshold. In a preferred embodiment, the composition is used to treat male or female sexual dysfunction, and more preferably erectile dysfunction. When used as therapeutic agents, the compositions of the present invention may be administered by any appropriate route that is known in the art. For example, they may be administered by the oral, buccal, sublingual, rectal, intravaginal, nasal, pulmonary or transdermal routes. Alternatively, they may be given by injection, including intravenous, subcutaneous and intramuscular injection. The amount given will be determined by the attending physician taking into consideration all appropriate factors. Generally a single dose will comprise between 0.1 mg and 1000mg, preferably between 1mg and 250mg, of active compound. The dose may be given on a single occasion or repeatedly. When given repeatedly, it may be given at regular intervals, such as once, twice or three times daily, or on demand, according to the condition .being treated. For long-term treatment an alternative to repeated dosing may be the administration of a depot dose. For this method of administration the active agent is generally introduced into a matrix of biodegradable polymer, such as a copolymer of lactic and glycolic acids, and the formulation is given either s.c. or i.m. so as to form a deposit from which the active agent is released as the polymer degrades. The foregoing description is further illustrated in the following examples, which are intended to demonstrate the application of the invention but not to limit the scope thereof. EXAMPLES The following abbreviations have been used: Bu butyl - alkyl residues may be further denoted as n (normal, i.e. unbranched), i (iso) and t (tertiary) DIEA A/,A/-diisopropylethylamine DMF dimethylformamide Et ethyl EtOAc ethyl acetate HOBt 1-hydroxybenzotriazole HPLC high pressure liquid chromatography h hour(s) Me methyl MS mass spectrum NMR nuclear magnetic resonance spectrum - NMR spectra were recorded in CDCI3 unless otherwise indicated OVA ornithine vasotocin analogue pet. ether petroleum ether boiling in the range 60-80°C Ph phenyl Pn pentyl Pr propyl THF tetrahydrofuran WSCD water-soluble carbodiimide (A/-ethyl-A/'-(3-dimethylaminopropyl)carbodiimide hydrochloride Examples 1-9 describe the synthesis of intermediates. Compounds according to the present invention are described in Examples 10 to 134. Example 1 1 -Benzyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (Figure Removed) 1A: Ethyl 5-amino-1-benzylpyrazole-4-carboxylate Benzylhydrazine dihydrochloride (4.29g, 22mmol) was added to a solution of ethyl (ethoxymethylene)cyanoacetate (3.38g, 20mmol) and triethylamine (6.15ml, 44mmol, 2eq) in ethanol (40ml) and the mixture was heated at reflux for 18h. The solvent was removed in vacua and the residue was purified by flash chromatography on silica gel (eluant 60% pet. ether/40% ethyl acetate) to yield a pale yellow solid identified as ethyl 5-amino-1-benzylpyrazole-4-carboxylate (4.3g, 88%). 1B: Ethyl 1-benzyl-5-(2'-nitrophenylamino)pyrazole-4-carboxyIate Sodium hydride (60% dispersion in oil, 520mg, 13mmol) was added portionwise to a suspension of ethyl 5-amino-1-benzylpyrazole-4-carboxylate (2.2g, 9mmol) in anhydrous THF (30ml) at 0°C. The mixture was allowed to warm to room temperature and stirred for 2h then 1-fluoro-2-nitrobenzene (1.26g, 9mmol) was added and the resultant deep purple suspension was stirred at room temperature for 18h. 1M KHSO4 was added to quench the reaction and the solvent was removed in vacua. The residue was dissolved in ethyl acetate and the solution was washed with 0.3M KHSO4l sat. NaHCO3 and brine, dried over Na2SO4 and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 75% pet. ether/25% ethyl acetate) to yield ethyl 1-benzyl-5-(2'-nitrophenylamino)pyrazole-4-carboxylate (2.5g, 76%). MS [M+H]+ 366.8 1C: Ethyl 5-(2'-aminopheny1amino)-1-benzylpyrazole-4-carboxyIate Ethyl 1-benzyl-5-(2'-nitrophenylamino)pyrazole-4-carboxylate (2.5g, 6.8mmol) was dissolved in ethyl acetate/ethanol (1:1, 100ml) and hydrogenated over 10% Pd/C catalyst for 70 minutes. The mixture was filtered through Celite® filter agent and the filtrate was concentrated in vacua to give a white solid identified as ethyl 5-(2'-aminophenylamino)-1-benzylpyrazole-4-carboxylate (1.5g, 86%). MS [M+H]+ 337.2 1D: 1-Benzyl-4,10-dihydropyrazolo[5,4-fa][1,5]benzodiazepin-4(5H)-one A solution of ethyl 5-(2'-aminophenylamino)-1-benzylpyrazole-4-carboxylate (1.75g, 5.2mmol) in acetic acid/ 2-propanol (1:9, 40ml) was heated at reflux for 3 days. The solvent was removed in vacua and the residue was azeotroped with toluene to give an off-white solid that was purified by flash chromatography on silica gel (eluant 35% pet. ether/65% ethyl acetate) to yield a white solid identified as 1-benzyl-4,10-dihydro-pyrazolo[5,4-)b][1,5]benzodiazepin-4(5H)-one (780mg, 52%). MS[M+H]+291.1 1E: 1 -Benzyl-4,10-dihydropyrazolo[5,4-6][1,5]benzodiazepine LiAIH4 (365mg, 10mmol) was added portionwise to a suspension of 1-benzyl-4,10-dihydropyrazolo[5,4-Jb][1,5]benzodiazepin-4(5H)-one (780mg, 2.7mmol) in anhydrous THF (15ml) at 0°C over 10min. The resulting suspension was heated at reflux for 18h, then allowed to cool to room temperature. A further portion of LiAIH4 (90mg, 2.5mmol) was added and the mixture was heated at refluxed for 3h. The mixture was cooled to 0°C, 35% ammonia solution (1ml) was added dropwise over 10min and the mixture was stirred at room temperature for 1 h. The resulting suspension was filtered through Celite® filter agent and the filtrate was concentrated in vacua to give a white solid identified as 1-benzyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (450mg, 60%). MS [M+H]+ 276.9 Example 2 1-Methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-/j][1,4]diazepine (Figure Removed) 2A: Ethyl 1 -methyl-2-(3'-nitro-2'-pyridylamino)pyrazole-4-carboxylate Sodium hydride (60% dispersion in oil, 600mg, 15mmol) was added portionwise to a suspension of ethyl 5-amino-1-methylpyrazole-4-carboxylate (1.69g, 10mmol) in anhydrous THF (15ml) at 0°C. The mixture was stirred for 2h at room temperature then 2-chloro-3-nitropyridine (1.58g, 10mmol) was added and the resulting deep red suspension was stirred at room temperature for 18h. 1M KHSO4 was added to quench the reaction and the solvent was removed in vacua. The residue was dissolved in ethyl acetate and the solution was washed with 0.3M KHSO4, sat. NaHCO3 and brine, dried over Na2SO4 and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 30% pet. ether/70% ethyl acetate) to give ethyl 1-methyl-2-(3'-nitro-2'-pyridylamino)pyrazole-4-carboxylate (1.95g, 67%). MS [M+Hf 292.0 2B: Ethyl 2-(3'-amino-2'-pyridylamino)-1-methylpyrazole-4-carboxylate A solution of ethyl 1-methyl-2-(3'-nitro-2'-pyridylamino)pyrazole-4-carboxylate (1.95g, 6.7mmol) in ethanol (100ml) was hydrogenated over 10% Pd/C catalyst for 3h. The reaction mixture was filtered through Celite® filter agent and the filtrate was concentrated in vacua to give a white solid identified as ethyl 2-(3'-amino-2'-pyridylamino)-1-methyl-pyrazole-4-carboxylate (1.5g, 86%). 2C: 1-WlethyI-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-b][1,4]diazepin-4(5H)-one A solution of ethyl 2-(3'-amino-2'-pyridylamino)-1-methylpyrazole-4-carboxylate (1.5g, 5.75mmol) in acetic acid/2-propanol (1:9, 50ml) was heated at reflux for 3 days. The solvent was removed in vacuo and the residue was azeotroped with toluene. The residue was purified by recrystallization from ethanol and then flash chromatography on silica gel (eluant 95% chloroform/4% methanol/1% acetic acid) to give a white solid identified as l-methyM.IO-dihydropyrazolo^.S-cJpyrido^.S-bni ,4]diazepin-4(5/-/)-one (560mg, 45%). 2D: 1-Methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-)Sj][1,43diazepine LiAIH4 (365mg, 10mmol) was added portionwise to a suspension of 1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-Jb][1,4]diazepin-4(5/^)-one (560mg, 2.6mmol) in anhydrous THF (30ml) at 0°C over 10 minutes. The resulting suspension was heated at reflux for 18h. The reaction was cooled to 0°C and 35% ammonia solution (1ml) was added dropwise over 10 minutes, then the mixture was stirred at room temperature for 1h. The resulting suspension was filtered through Celite® filter agent and the filtrate was concentrated in vacuo to give a white solid identified as 1-methyl-4,10-dihydro-pyrazolo[4,5-c]pyrido[2,3Hb][1,4]diazepine (410mg, 78%). MS [M+H]+202.1. Example 3 tert-Butyl 4-aminomethyl-3-chlorobenzoate (Figure Removed) 3A: tert-Butyl 3-chloro-4-methylbenzoate Thionyl chloride (11ml, 150mmol) was added to a suspension of 3-chloro-4-methyl-benzoic acid (5.12g, SOmmol) in toluene (25ml) and the mixture was heated at reflux for 2h. The solvent was removed in vacua and the residue was azeotroped with toluene three times, then dissolved in anhydrous THF (40ml) and cooled to 0°C. Lithium tert-butoxide (2.4g, SOmmol) was added and the mixture was stirred at room temperature for 3 days. Water (5ml) was added and the solvent was removed in vacua. The residue was dissolved in ethyl acetate. The solution was washed with 0.3M KHSO4, sat. NaHCO3 and brine, dried over Na2SO4 and concentrated in vacua to give a pale yellow gum identified as te/f-butyl 3-chloro-4-methylbenzoate (5.4g, 79%). 3B: tert-Butyl 4-bromomethyl-3-chlorobenzoate A/-Bromosuccinimide (4.27g, 24mmol) and 2,2'-azonb/s(2-methylpropionitrile) (394mg, 2.4mmol) were added to a solution of te/f-butyl 3-chloro-4-methylbenzoate (5.4g, 23.8mrnol) in carbon tetrachloride (75ml) and the mixture was heated at reflux for 18h. The solvent was removed in vacua and the residue was purified by flash chromatography on silica gel (eluant 95% pet.ether/5% ethyl acetate) to give a white solid identified as te/f-butyl 4-bromomethyl-3-chlorobenzoate (5.7g, 78%). 3C: tert-Butyl 4-aminomethyl-3-chlorobenzoate Ethanol (100ml) was saturated with ammonia, then terf-butyl 4-bromomethyl-3-chloro-benzoate (5.7g, 18.7mmol) was added and the mixture was stirred at room temperature for 2h. The solvent was removed in vacuo and the residue was triturated with diethyl ether to give a white solid identified as te/f-butyl 4-aminomethyl-3-chlorobenzoate (4.1g, 91%). Example 4 4-(fert-Butyloxycarbonylaminomethyl)-3-(Figure Removed) H 4A. Methyl 4-bromomethyl-3-chlorobenzoate To a solution of methyl 3-chloro-4-methylbenzoate (5.0g, 27.1mmol) in carbon tetrachloride (50ml) were added A/-bromosuccinimide (5.8g, 32.0mmol) and 2,2'-azo-£»/s(2-methylpropionitrile) (0.442g, 2.70mmol). The mixture was heated at reflux for 18h, then allowed to cool to room temperature and concentrated in vacuo. The residue was purified by flash chromatography on silica (eluant pet. ether -» 5% ethyl acetate/95% pet. ether) to give an oil identified as methyl 4-bromomethyl-3-chlorobenzoate (5.96g, 84%). 4B. 4-(fert-Butyloxycarbonylaminornethyl)-3-chlorobenzoic acid To a saturated solution of ammonia in ethanol (170ml) was added methyl 4-bromomethyl-3-chlorobenzoate from Example 4A (5.5g, 20.9mmol). The mixture was stirred at room temperature for 1h and then concentrated in vacuo. The residue was triturated with diethyl ether and the resultant white crystals were filtered off and washed with more diethyl ether. To a solution of this solid in water (100ml) were added solutions of di-te/t-butyl dicarbonate (5.0g, 23.0mmol) in dioxan (100ml) and sodium hydroxide (1.86g, 46.0mmol) in water (100ml). The mixture was stirred at room temperature for 18h and then concentrated in vacuo. The aqueous residue was acidified with citric acid and extracted with chloroform/2-propanol. The organic layer was washed with water, dried over MgSO4, and concentrated in vacuo to give a white solid identified as 4-(terf-butyloxy-carbonylaminomethyl)-3-chlorobenzoic acid (2.8g, 67%). Example 5 4-(fert-Butyloxycarbonylaminomethyl)-3-nitrobenzoic acid (Figure Removed) 4-Bromomethyl-3-nitrobenzoic acid (4.75g, 18.2mmol) was reacted following the method of Example 4B to give a yellow solid identified as 4-(te/t-butyloxycarbonylarninomethyl)-3-nitrobenzoic acid (2.6g, 49%). Example 6 4-Cyano-3-methylbenzoic acid(Figure Removed) To a solution of 4-brorno-2-methylbenzonitrile (2.0g, 10.2mmol) in THF (100ml) at-78°C under a nitrogen atmosphere was added dropwise a 2.5M solution of n-butyl lithium (4.48ml, 11.2mmol). The mixture was stirred at -78°C for 1h and then poured onto solid carbon dioxide (5g) in THF (50ml). The mixture was allowed to warm to room temperature. Water was added (200ml) and the mixture was extracted with diethyl ether (3 times). The aqueous layer was acidified by addition of concentrated HCI and extracted with chloroform (3 times). The combined chloroform extracts were washed with water, dried over MgSO4, and concentrated in vacua to give a white solid identified as 4-cyano-3-methylbenzoic acid (1.2g, 73%). (Figure Removed) 4-Bromo-3-methylbenzonitrile (2.0g, 10.2mmol) was reacted following the method of Example 6. The product was triturated with hexane to give a yellow solid identified as 4-cyano-2-methylbenzoic acid (0.96g, 59%). Example 8 4-(terf-ButyloxycarbonylaminomethyI)-2-fluorobenzoic acid (Figure Removed) 8A. 2-Fluoro-4-methylbenzoic acid 4-Bromo-3-fluorotoluene (8.33g, 44.07mmol) was reacted following the method of Example 6 to give a white solid identified as 2-fluoro-4-methylbenzoic acid (4.89g, 72%). 8B. Methyl 2-fluoro-4-methylbenzoate To a solution of 2-fiuoro-4-methylbenzoic acid (6.04g, 39.18mmol) in toluene (80ml) was added thionyl chloride (65ml, 89.11mmol). The mixture was heated at reflux for 2.5h, cooled and concentrated in vacua. The residue was dissolved in dichloromethane (50ml) and methanol (50ml) was added. The mixture was stirred at room temperature for 2.5h and then concentrated in vacua. The residue was dissolved in dichloromethane (100ml), washed with saturated sodium bicarbonate solution and brine, dried over MgSO4, and concentrated in vacua to give a tan solid identified as methyl 2-fluoro-4-methylbenzoate (5.07g, 77%). 8C. Methyl 4-bromomethyl-2-fluorobenzoate Methyl 2-fluoro-4-methylbenzoate (5.07g, 30.16mmol) was reacted following the method of Example of 4A. The product was purified by flash chromatography on silica (eluant 20% ethyl acetate/ 80% pet. ether) to give an oil identified as methyl 4-bromomethyl-2-fluorobenzoate (5.9g, 80%). 8D. 4-(tert-Butyloxycarbonylaminomethyl)-2-fluorobenzoic acid Methyl 4-bromomethyl-2-fluorobenzoate (5.9g, 24.13mmol) was reacted following the method of Example 4B. The product was recrystallised from dioxan/pet. ether to give white crystals identified as 4-(terf-butyloxycarbonylaminomethyl)-2-fluorobenzoic acid (2.46g, 38%). Example 9 4-Cyano-3,5-dimethylbenzoic acid (Figure Removed) 9A. 4-Bromo-2,6-dimethylbenzonitrile 4-Brorno-2,6-dimethylaniline (4.49g, 22.4mmol) was taken up in water (25ml) and concentrated hydrochloric acid (8.0ml) was added. The mixture was sonicated to form a fine suspension and then cooled to 0°C. A solution of sodium nitrite (1.67g, 24.2mmol) in water (5ml) was then added dropwise so as to maintain the temperature of the reaction between 0-5°C. The mixture was stirred at 0-5°C for 30 minutes and then neutralised by addition of solid sodium bicarbonate. The resulting solution was then added portionwise to a solution of copper cyanide (2.42g, 27.0mmol) and potassium cyanide (3.65g, 56.1mmol) in water (25ml) at 70°C. The mixture was stirred at 70°C for 30 minutes, allowed to cool and then extracted with toluene (2 times). The combined extracts were washed with water and brine, dried over MgSO4, and concentrated in vacua. The residue was purified by flash chromatography on silica (eluant 5% ethyl acetate/ 95% pet. ether) to give an orange solid identified as 4-bromo-2,6-dimethylbenzonitrile (3.2g, 68%). 9B. 4-Cyano-3,5-dimethy!benzoic acid 4-Bromo-2,6-dimethylbenzonitrile (3.20g, 15.2mmol) was reacted following the method of Example 6 to give a tan solid identified as 4-cyano-3,5-dimethylbenzoic acid (1.5g, 56%). Example 10 4-(3-Methyl-4-(piperazine-1-carbonylaminomethyl)benzoyl)-5,6,7,8-tetrahydrothieno[3,2-/3]azepine hydrochloride (Figure Removed) 10A: 4-(3-Methyl-4-cyanobenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine Thionyl chloride (5ml, 68.55mmol) was added to a stirred suspension of 4-cyano-3-methylbenzoic acid (1.43g, 8.90mmol) in dichloromethane (20ml). The mixture was heated at reflux for 2h, cooled to room temperature and concentrated in vacua. The residue was azeotroped with dichloromethane then dissolved in dichloromethane 20ml. The resulting solution was slowly added to a stirred solution of 5,6,7,8-tetrahydrothieno[3,2-b]azepine (1.36g, 8.90mmol) and triethylamine (3.70ml, 26.54mmol) n dichloromethane (30ml). The mixture was stirred at room temperature for 24h, washed with 1M KHSO4l saturated NaHCO3 and brine, then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 25% EtOAc/pet. ether) to give a brown solid identified as 4-(3-methyl-4-cyanobenzoyl)-5,6,7,8-tetrahydrothieno[3,2-6jazepine (1.70g, 71%). 10B: ^(^Aminomethyl-S-methylbenzoyO-S.ej.S-tetrahydrothienop.Z-fajazepine Cobalt(ll) chloride hexahydrate (2.84g, 11.94mmol) was added to a solution of 4-(3-methyl-4-cyanobenzoyl)-5,6,7,8-tetrahydrothieno[3,2Hb]azepine (1.70g, 5.70mmol) in methanol (70ml) at 0°C. Sodium borohydride (2.22g, 58.68mmol) was added portionwise at 0°C and the mixture was stirred at 0°C for SOmin then at room temperature for 2h. Saturated ammonium chloride was then added and the mixture was stirred for SOmin then concentrated in vacua. The residue was azeotroped with toluene then extracted with chloroform. The extracts were washed with brine and concentrated in vacua to give a white solid identified as 4-(4-aminomethyl-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine (1.12g, 65%). 10C: 4-(4-(4-{fe/t-ButyloxycarbonyI)piperazine-1-carbonylaminomethyl)-3-methyl-benzoyl)-5,6,7,8-tetrahydrothieno[3>2-d]azepine 1,1'-Carbonyldiimidazole (234mg, 1.45mmol) was added to a solution of 4-(4-amino-methyl-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-Jb]azepine (400mg, 1.33mmol) and DIEA (0.3ml, 1.72mmol) in DMF (20ml) and the mixture was stirred at room temperature for SOmin. terf-Butyl piperazine-1-carboxylate (281mg, 1.50mmol) was added and the mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was taken up in chloroform and the solution was washed with 1M KHSO4 and brine, then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 75% EtOAc/pet. ether) to give a white solid identified as 4-(4-(4-(terf-butyloxycarbonyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine (588mg, 86%). 10D: 4-(3-MethyI-4-(piperazine-1-carbonylaminomethyl)benzoyl)-5,6,7,8-tetrahydrothieno[3,2-/j]azepine hydrochloride A solution of 4-(4-(4-(te/t-butyloxycarbonyl)piperazine-1-carbonylaminomethyl)-3-methyl-benzoyl)-5,6,7,8-tetrahydrothieno[3,2-d]azepine (588mg, 1.15mrnol) in 4N HCI/dioxan (10ml) was stirred at room temperature for SOmin then concentrated in vacua. The residue was dissolved in acetonitrile/water and lyophilised to give a white solid identified as 4-(3-methyl-4-(piperazine-1-carbonylaminomethyl)benzoyl)-5,6l7,8-tetrahydrothieno-[3,2-i>]azepine hydrochloride(393mg, 76%). 1H NMR: d6-DMSO 5 1.60-1.74 (2H, m), 1.82-1.94 (2H, m), 2.17 (3H, s), 2.86-2.95 (2H, m), 2.96-3.10 (4H, m), 3.35-3.45 (2H, m), 3.50-3.64 (4H, m), 4.16 (2H, s), 6.26 (1H, br s), 6.85-7.10 (4H, m), 7.24 (1H, br s), 9.28 (1H, brs) ppm. MS:[M+Hf = Example 11 5-(4-(4-CycIopropylmethylpiperazine-1-carbonylaminomethyI)-3-methyIbenzoyl)-1- methyMJO-dihydropyrazolol^-bJII.JjJbenzodiazepine (Figure Removed) 11 A: S^-Cyano-S-methylbenzoylJ-l-methyM.IO-dihydropyrazolotS^-Jblll.S]-benzodiazepine Thionyl chloride (1.8ml, 27mmol) was added to a stirred suspension of 4-cyano-3-methyl-benzoic acid (1.29g, S.Ommol) in toluene (25ml). The mixture was heated at reflux for 2hr, cooled to room temperature and concentrated in vacua. The residue was azeotroped with toluene then dissolved in dichloromethane (10ml). The resulting solution was added to a stirred suspension of 1-methyl-4,10-dihydropyrazolo[5,4-6][1,5]benzodiazepine (1.6g, 8mmol) and triethylamine (1.4ml, 10mmol) in dichloromethane (15ml). The mixture was stirred overnight at room temperature then concentrated in vacua. The residue was partitioned between chloroform and 0.3M KHSO4. The aqueous phase was extracted with chloroform/2-propanol (80:20). The combined organic phases were washed with sat. NaHCO3 and brine, dried over Na2SO4 and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 5% methanol/chloroform) to give a pale yellow solid identified as 5-(4-cyano-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-6][1,5]benzodiazepine (2.4g, 87%). 11B: 5-(4-Aminomethyl-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]-benzodiazepine Cobalt(ll) chloride hexahydrate (1.59g, 6.7mmol) was added to an ice-cold solution of 5-{4-cyano-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (1.15g, 3.35mmol) in methanol (35ml). Sodium borohydride (1.27g, 33.5mmol) was added portionwise at 0°C and the mixture was stirred at RT for 1 hr, then quenched with 1M KHSO4 and concentrated in vacua. The aqueous residue was diluted with 1M KHSO4 (40ml) and filtered through Celite® filter agent. The filtrate was washed with diethyl ether (2 x 50ml) then basified with 2M NaOH and extracted with chloroform. The organic phase was dried over Na2SC>4 and concentrated in vacua to give a pale brown solid identified as 5-(4-aminomethyl-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo-[5,4-d][1,5]benzodiazepine (745mg, 64%). 11C: 5-(4-(4-{fert-Butyloxycarbonyl)piperazine-1-carbonylaminomethyl)-3-methyl-benzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine 1,1'-Carbonyldiimidazole (76mg, 0.47mmol) was added to a solution of 5-(4-(aminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-jb][1,5]benzo-diazepine (150mg, 0.43mmol) and DIEA (0.1ml, 0.57mmol) in DMF (10ml). The solution was stirred for 30min, terf-butyl piperazine-1-carboxylate (91mg, 0.49mmol) was added and stirring was continued for 72h. The mixture was concentrated in vacua and the residue was taken up in chloroform. The solution was washed with water and brine, dried and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 100% EtOAc then 10%methanol/EtOAc) to give a white solid identified as 5-(4-(4-(tert-butyloxycarbonyl)piperazine-1 -carbonylaminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (160mg, 66%). 11D: l-Methyl-B^S-methyW-tpiperazine-l-carbonylaminomethyO-benzoyO^.IO-dihydropyrazolo[5,4-fa][1,5]benzodiazepine hydrochloride A solution of 5-(4-(4-(fert-butyloxycarbonyl)piperazine-1-carbonylaminomethyl)-3-methyl-benzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (160mg, 0.29mmol) in 4N HCI/dioxan (15ml) was stirred at room temperature for 30min then concentrated in vacua. The residue was azeotroped with diethyl ether to give a white solid identified as 1 -methyl-5-(3-methyl-4-(piperazine-1 -carbonyIaminomethyl)-benzoyl)-4,10-dihydro-pyrazolo[5,4-Jb][1,5]benzodiazepine hydrochloride (130mg, 90%). 11E: 5-(4-(4-Cyclopropylmethylpiperazine-1 -carbonylaminomethyl)-3-methyi-benzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine To a solution of 1-methyl-5-(3-methyl-4-(piperazine-1-carbonylaminomethyl)-benzoyl)-4,10-dihydropyrazolo[5,4-/b][1,5]benzodiazepine hydrochloride (100mg, 0.20mmol) and triethylamine (0.5ml, 3.59mmol) in THF (10ml) were added cyclopropanecarboxaldehyde (14mg, 0.20mmol) and sodium cyanoborohydride (15mg, 0.24mmol) and the resulting mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was dissolved in ethyl acetate and the resulting solution was washed with saturated NaHCO3, water and brine, dried and concentrated in vacua. The residue was purified by flash chrornatography on silica gel (eluant 10% methanol/EtOAc) to give a white solid identified as 5-(4-(4-cyclopropylmethylpiperazine-1-carbonylaminomethyl)-3-methylbenzoyO-l-methyW.IO-dihydropyrazolotS^-dltl.Slbenzodiazepine (35mg, 35%). 1H NMR: d MS: [M+H]+ = 514.3 Example 12 5-{4-(4-Benzylpiperazine-1-carbonylaminomethyl)-3-methyIbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-/b][1,5]benzodiazepine (Figure Removed) To a solution of 1-methyl-5-(3-methyl-4-(piperazine-1-carbonylaminomethyl)-benzoyl)-4,10-dihydropyrazolo[5,4-Jb][1,5]benzodiazepine hydrochloride (100mg, 0.20mmol) and triethylamine (0.5ml, 3.59mmol) in THF (10ml) were added benzaldehyde (21 mg, 0.20mmol) and sodium cyanoborohydride (15mg, 0.24mmol) and the resulting mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was dissolved in ethyl acetate and the resulting solution was washed with saturated NaHCO3l water and brine, dried and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 5% methanol/EtOAc) to give a white solid identified as 5-(4-(4-benzylpiperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-d][1,5]benzodiazepine (37mg, 34%). 1H NMR: 8 2.10 (3H, s), 2.36-2.48 (4H, m), 3.29-3.44 (4H, m), 3.48-3.51 (2H, m), 3.76 (3H, s), 3.96 (1H, d, J=14.6Hz), 4.22-4.28 (2H, m), 4.61-4.68 (1H, m), 5.88 (1H, d, J=14.6Hz), 6.46 (1H, s,) 6.62-6.74 (2H, m), 6.82-6.96 (3H, m), 6.98-7.11 (2H, m), 7.19-7.34 (5H, m) ppm. MS: [M+H]+ = 550.2 Example 13 5-(4-(4-(3-Hydroxybenzyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1- methyl-4,10-dihydropyrazoIo[5,4-Jb][1,5]benzodiazepine (Figure Removed) 13A: 3-(fert-ButyldimethylsiIyloxy)toIuene terf-Butyldimethylsilyl chloride (S.OOg, 22.00mmol) was added to a solution of m-cresol (2.00g, 18.00mmol) and triethylamine (4ml, 28.7mmol) in dichloromethane (50ml) at 0°C. The mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 10% EtOAc/pet. ether) to give a colourless oil identified as 3-(te/f-butyldimethylsilyloxy)toluene (3.60g, 88%). 13B: 3-{ferf-Butyldirnethylsilyloxy)benzyl bromide A/-Bromosuccinimide (2.90g, 16.20mmol) and AIBN (266mg, 1.62mmol) were added to a stirred solution of 3-(terf-butyldimethylsilyloxy)toluene (3.60g, 16.20mmol) in carbon tetrachloride (120ml) and the mixture was heated at reflux for 24h, then allowed to cool to room temperature and concentrated in vacuo. The residue was purified by flash chromatography on silica gel (eluant cyclohexane) to give a colourless oil identified as 3-(te/f-butyldimethylsilyloxy)benzyl bromide (2.45g, 50%). 13C: tert-Butyl 4-{3-hydroxybenzyl)piperazine-1-carboxylate Sodium hydride (406mg, 60% dispersion in oil, 10.15mmol) was added portionwise to a stirred solution of fe/t-butyl piperazine-1-carboxylate in DMF (50ml) at 0°C. The mixture was allowed to warm to room temperature over 1h, then a solution of 3-(tert-butyldimethylsilyloxy)benzyl bromide (2.44g, 8.10mmol) in DMF (10ml) was added dropwise and the mixture was stirred at room temperature for 24h. Water was added and the mixture was stirred for SOmin then poured into EtOAc. The organic phase was washed with saturated NaHCO3 and brine, then concentrated in vacuo. The residue was purified by flash chromatography on silica gel (eluant 40% EtOAc/pet. ether) to give a light brown oil identified as tert-butyl 4-(3-hydroxybenzyl)piperazine-1-carboxylate (2.00g, 84%). 13D: 1-(3-HydroxybenzyI)piperazine dihydrochloride A solution of fe/t-butyl 4-(3-hydroxybenzyl)piperazine-1-carboxylate (1.94g, 6.60mmol) in 4N HCI/dioxan (10ml) was stirred at room temperature for SOmin then concentrated in vacuo. The residue was triturated with diethyl ether to give a white solid identified as 1-(3-hydroxybenzyl)piperazine dihydrochloride (1.10g, 63%). 13E: 5-(4-(4-(3-Hydroxybenzyl)piperazine-1-carbonyIaminomethyI)-3-methyl-benzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine 1,1'-Carbonyldiimidazole (15mg, 0.09mmol) was added to a stirred solution of 5-(4-(aminomethyl)-3-methyibenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-d][1,5]benzo-diazepine (31mg, 0.09mmol) and DIEA (0.1ml 0.57mmol) in DMF (5ml). The solution was stirred for 1h, 1-(3-hydroxybenzyl)piperazine dihydrochloride (27mg, O.IOmmol) was added and stirring was continued at room temperature for 24h. The mixture was concentrated in vacuo and the residue was taken up in EtOAc. The solution was washed with saturated NaHCO3 and brine, then concentrated in vacuo. The residue was purified by flash chromatography on silica gel (eluant 20% methanol/EtOAc) to give a white solid identified as 5-(4-(4-(3-hydroxybenzyl)piperazine-1-carbonylaminomethyI)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-6][1,5]benzodiazepine (45mg, 90%). 1H NMR: 6 2.15 (3H, s), 2.41 (4H, t, J=4.7Hz), 3.40 (4H, t, J=4.7Hz), 3.46 (2H, s), 3.80 (3H, s), 3.97 (1H, d, J=14.6Hz), 4.22 (2H, s), 4.90 (1H, m), 5.78 (1H, d, J=14.6Hz), 6.62-6.79 (5H, m), 6.99 (2H, s), 7.03-7.27 (6H, m) ppm. MS: [M+H]+ = 566.1 Example 14 5-{4-(4-(3-Hydroxymethylbenzyl)piperazine-1-carbonylaminomethyl)-3-methyl- benzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-/)][1,5]benzodiazepine (Figure Removed) 14A: tert-Butyl 4-(3-(methyIoxycarbonyl)benzyl)piperazine-1-carboxylate Methyl 3-(bromomethylbenzoate) (1.23g, 5.37mmol) was added to a stirred solution of terf-butyl piperazine-1-carboxylate (1.00g, 5.37mmol) and triethylamine (1.50ml, 10.74mmol) in dichloromethane (20ml). The solution was stirred at room temperature for 24h then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant EtOAc) to give a white solid identified as terf-butyl 4-(3-(methyloxycarbonyl)benzyl)piperazine-1-carboxylate (1.55g, 86%). 14B: terf-Butyl 4-(3-carboxybenzyl)piperazine-1-carboxyIate Lithium hydroxide monohydrate (339mg, 9.27mmol) was added to a solution of terf-butyl 4-(3-(methyloxycarbonyl)benzyl)piperazine-1-carboxylate (1.55g, 4.63mmol) in THF (10ml) and water (2ml). The solution was stirred at room temperature for 24h then acidified to pH 5 with 0.3M KHSO4 and extracted successively with chloroform and dichloromethane. The combined extracts were concentrated in vacua to give a white solid identified as te/f-butyl 4-(3-carboxybenzyl)piperazine-1-carboxylate (1.09g, 74%). 14C: fert-Butyl 4-(3-{hydroxymethyl)benzyl)piperazine-1-carboxyIate Isobutyl chloroformate (0.47ml, 3.64mmol) was slowly added to an ice-cold solution of te/f-butyl 4-(3-carboxybenzyl)piperazine-1-carboxylate (1.06g, 3.31 mmol) and N-methylmorpholine (0.80ml, 7.28mmol) in THF (15ml). The solution was stirred at 0°C for 45min and then filtered. The filtrate was added to an ice-cold solution of sodium borohydride (313mg, 8.27mmol) in water (10ml). The stirred mixture was allowed to warm to room temperature over 2h and then concentrated in vacua. The residue was taken up in EtOAc and the solution was washed with water and brine then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant-EtOAc) to give a white solid identified as te/f-butyl 4-(3-(hydroxymethyl)benzyl)piperazine-1-carboxylate (230mg, 23%). 14D: 1-(3-(Hydroxymethyl)benzyl)piperazine dihydrochloride A solution of terf-butyl 4-(3-(hydroxymethyl)benzyl)piperazine-1-carboxylate (230mg, 0.75mmol) in 4N HCI/dioxan (10ml) was stirred at room temperature for 45min then concentrated in vacua. The residue was azeotroped with toluene to give a white solid identified as 1-(3-(hydroxymethyl)benzyl)piperazine dihydrochloride (158mg, 75%). 14E: 5-(4-(4-(3-Hydroxymethylbenzyl)piperazJne-1-carbonylaminomethyl)-3-methyl-benzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine 1,1'-Carbonyldiimidazole (20mg, 0.12mmol) was added to a solution of 5-(4-(aminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-£»][1,5]benzo-diazepine (35mg, O.IOmmol) in DMF (3ml). The solution was stirred for 1h, a solution of 1-(3-(hydroxymethyl)benzyl)piperazine dihydrochloride (31mg, O.Hmmol) and DIEA (54)11, O.SOmmol) in DMF (2ml) was added and the mixture was stirred at room temperature for 24h then concentrated in vacua. The residue taken up in chloroform and the solution was washed with brine and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 7% methanol/chloroform) to give a white solid identified as 5-(4-(4-(3-hydroxymethylbenzyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-6][1,5]benzodiazepine (27mg, 50%). 1H NMR: 5 2.00 (3H, s), 2.32-2.36 (4H, m), 3.32-3.45 (4H, m), 3.46 (2H, s), 3.63 (3H, s), 3.91 (1H, d, J=14.6Hz), 4.10-4.20 (1H, m), 4.66 (2H, s), 5.28-5.29 (1H, m), 5.80 (1H, d, J=14.3Hz), 6.50-7.30 (15H, m) ppm. MS: [M+H]+ = 580.3 Example 15 1-Methyl-5-(3-methyl-4-(4-(4-picolyl)pipera2ine-1-carbonylaminomethyl)benzoyl)-4,10-dinydropyrazolo[5,4-/j][1,5]benzodiazepine (Figure Removed) MS: [M+H]+ = 551.1 Example 16 5^4-(4-(2-Hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyI)-1- methyl-4,10-dihydropyrazolo[5,4-Jb][1,5]benzodiazepine (Figure Removed) 1,1'-Carbonyldiimidazole (20mg, 0.19mmol) was added to a solution of 5-(4-(aminomethyO-S-methylbenzoyO-l-methyW.IO-dihydropyrazolotS^-^tl.Slbenzo-diazepine (31 mg, O.OSmmol) in DMF (3ml). The solution was stirred at room temperature for 1h, a solution of 1-(2-hydroxyethyl)piperazine (13mg, O.IOmmol) in DMF (2ml) was added and stirring was continued for 72h. The solution was concentrated in vacua and the residue was partitioned between chloroform and brine. The organic layer was separated and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 7% methanol/chloroform) to give a white solid identified as 5-(4-(4-(2-hydroxyethyl)piperazine-1 -carbonylaminomethyl)-3-methyl-benzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-jb][1,5]benzodiazepine (22mg, 48%). 1H NMR: 8 2.09 (3H, s), 2.42-2.59 (6H, m), 2.91-3.01 (1H, m), 3.33-3.62 (6H, m), 3.67 (3H, s), 3.93-3.98 (1H, m), 4.20-4.23 (2H, m), 5.00-5.03 (1H, m), 5.84-5.90 (1H, m), 6.64-7.25 (9H, m) ppm. MS: [M+H]+ = 504.2 Example 17 1-MethyI-5-(3-methyl-4-(4-(3-(methylthio)propyl)piperazine-1-carbonylaminomethyl)-benzoyl)-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (Figure Removed) To a solution of 1-methyl-5-(3-methyl-4-(piperazine-1-carbonyiarninomethyl)-benzoyl)-4,10-dihydropyrazolo[5,4-/)][1,5]benzodiazepine hydrochloride (100mg, 0.20mmol) and triethylamine (0.5ml, 3.59mmol) in THF (10ml) were added 3-(methylthio)-propionaldehyde (21 mg, 0,20mmol) and sodium cyanoborohydride (15mg, 0.24mmol) and the resulting mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was dissolved in ethyl acetate and the resulting solution was washed with saturated NaHCO3, water and brine, dried and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 20% methanol/EtOAc) to give a white solid identified as 1-methyl-5-(3-methyl-4-(4-(3-(methylthio)-propyl)piperazine-1 -carbonylarninomethyl)benzoyl)-4,10-dihydropyrazolo[5,4-k][1,5]-benzodiazepine (41 mg, 38%). 1H NMR: 8 1.63-1.80 (3H, m), 2.04-2.12 (4H, m), 2.33-2.42 (6H, m), 2.48 (2H, t, J=6.7Hz), 3.29-3.39 (4H, m), 3.71 (3H, s), 3.93 (1H, d, J=14.4Hz), 4.12-4.30 (2H, m), 4.57-4.70 (1H, m), 5.85 (1H, d, J=14.6Hz), 6.44 (1H, s), 6.59-6.71 (2H, m), 6.83-6.88 (2H, m), 6.92-7.08 (2H, m), 7.14-7.27 (2H, m) ppm. MS: [M+H]+ = 548.0 Example 18 5-(4-(4-(2-Aminoethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl}-1-methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine dihydrochloride (Figure Removed) 18A: Benzyl 4-(2-hydroxyethyl)piperazine-1-carboxylate Benzyl chloroform ate (3.40ml, 24.00mmol) was slowly added to an ice-cold stirred solution of 1-(2-hydroxyethyl)piperazine (2.60g, 20.00mmol) and DIEA (7.0ml, 40.0mmol) in dichloromethane (75ml). The mixture was allowed to warm to room temperature and stirred for 24h then concentrated in vacuo. The residue was purified by flash chromatography on silica gel (eluant 6% methanol/chloroform) to give a colourless gum identified as benzyl 4-(2-hydroxyethyl)piperazine-1-carboxylate (4.80g, 91%). 18B: Benzyl 4-(2-bromoethyl)piperazine-1-carboxylate Carbon tetrabromide (7.23g, 21.80mmol) was added to an ice-cold stirred solution of benzyl 4-(2-hydroxyethy!)piperazine-1-carboxylate (4.80g, 18.20mmol) in dichloromethane (50ml). The solution was stirred for 5min, triphenylphosphine (5.95g, 22.70mmol) was added, and the mixture was allowed to warm to room temperature and stirred for 3h. Silica gel was added and the solvent was removed in vacuo. The residue was purified by flash chromatography on silica gel (eluant 50% EtOAc/pet. ether) to give a colourless gum identified as benzyl 4-(2-bromoethyl)piperazine-1-carboxylate (3.45g, 58%). 18C: Benzyl 4-(2-(fe/t-butyloxycarbonylamino)ethyl)piperazine-1-carboxylate Benzyl 4-(2-bromoethyl)piperazine-1-carboxylate (3.45g, 10.55mmol) was added to an ice-cold saturated solution of ammonia in ethanol (60ml). The mixture was allowed to warm to room temperature and stirred for 4h, then concentrated in vacuo. The residue was triturated with diethyl ether. The resultant solid was suspended in dichloromethane (75ml) and triethylamine (2.25ml, 16.00mmol). The suspension was cooled to 0°C and di-terf-butyl dicarbonate (2.40g, H.OOmmol) was added. The mixture was allowed to warm to room temperature and stirred for 24h then concentrated in vacua. The residue was taken up in EtOAc. The solution was washed with saturated NaHC03 and brine, then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 3% methanol/chloroform) to give a yellow gum identified as benzyl 4-(2-(fe/t-butyloxycarbonylarnino)ethyl)piperazine-1 -carboxylate (2.60g, 68%). 18D: te/t-Butyl 2-(1-piperazinyl)ethylcarbamate Hydrogen was passed through a degassed solution of benzyl 4-(2-(tert-butyloxycarbonylamino)ethyl)piperazine-1-carboxylate (2.60g, 7.16mmol) in methanol (50ml) containing 10% palladium on carbon (SOOmg) for 2h. The reaction mixture was filtered through Celite® and the filtrate was concentrated in vacua to give a yellow gum identified as te/t-butyl 2-(1-piperazinyl)ethylcarbamate (1.60g, 97%). 18E: 5-(4-(4-(2-(fert-Butyloxycarbonylaminoethyl)piperazine-1-carbonyIamino-methyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[5,4-Jb][1,5]benzodiazepine 1,1'-Carbonyldiimidazole (25mg, 0.15mmol) was added to a solution of 5-(4-(aminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-6][1,5]benzo-diazepine (31 mg, 0.09mmol) and DIEA (0.1ml, 0.57mmol) in DMF (5ml). The solution was stirred for 1h, te/t-butyl 2-(1-piperazinyl)ethylcarbamate (22mg, O.IOmmol) was added and stirring was continued at room temperature for 24h. The mixture was concentrated in vacua and the residue was taken up in EtOAc. The solution was washed with saturated NaHCO3 and brine, then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 20% methanol/EtOAc) to give a white solid identified as 5-(4-(4-(2-(fert-butyloxycarbonylaminoethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-Jb][1,5]-benzodiazepine (44mg, 81%). 18F: 5-(4-(4-(2-AminoethyI)piperazine-1 -carbonylaminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-Jb][1,5]benzodiazepine dihydrochloride A solution of 5-(4-(4-(2-(te/f-butyloxycarbonylaminoethyl)piperazine-1-carbonylamino-methyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-/>][1,5]benzodiazepine (42mg, 0.07mmol) in 4N HCI/dioxan (5ml) was stirred at room temperature for SOmin then concentrated in vacua. The residue was dissolved in acetonitrile/water and lyophilised to give a white solid identified as 5-(4-(4-(2-aminoethyl)piperazine-1-carbonylaminomethyl)- 3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine dihydrochloride (37mg, 92%). 1H NMR: 5 2.17 (3H, s), 3.30-3.35 (4H, m), 3.41-3.50 (1H, m), 3.56-3.72 (4H, m), 4.00 (3H, s), 4.04 (1H, s), 4.26 (2H, s), 4.83-4.89 (2H, m), 5.88 (1H, d, J=15Hz), 6.83-6.84 (2H, m), 6.92-7.13 (4H, m), 7.15-7.28 (1H, m), 7.36 (1H, d, J=7.9Hz), 7.96 (1H, s) ppm. MS: [M+H]+ = 503.5 Example 19 1 -Methyl-5-(3-methyl-4-(4-methylperhydro-1,4-diazepine-1 - carbonylaminomethyl)benzoyl)-4,10-dihydropyrazolo[5,4-/j][1,5]benzodiazepine (Figure Removed) 1,1 '-Carbonyldiimidazole (37mg, 0.23mmol) was added to a solution of 5-(4-(aminomethyl)-3-methylbenzoyl)-1 -methyl-4,10-dihydropyrazolo[5,4-b][1,5]benzo-diazepine (75mg, 0.22mmol) in DMF (2ml). The solution was stirred for 1h, a solution of 1-methylhomopiperazine (27mg, 0.24mmol) and DIEA (31mg, 0.24mmol) in DMF (1ml) was added and stirring was continued for 24h. The mixture was concentrated in vacua and the residue was purified by chromatography on silica gel (eluant 30/2/1 — 1/1/1 chloroform/methanol/concentrated ammonia) to give a white solid identified as 1-methyl-5-(3-methyl-4-(4-rnethylperhydro-1,4-diazepine-1 -carbonylaminomethyl)benzoyl)-4,10-dihydropyrazolo[5,4-b][1,5]benzodiazepine (38mg, 36%). 1H NMR: 6 1.80-1.99 (2H, m), 2.10 (3H, s), 2.35 (3H, s), 2.51-2.69 (4H, m), 3.39 (2H, t, J=5.9Hz), 3.45-3.68 (2H, m), 3.63 (3H, s), 3.95 (1H, d, J=14.6Hz), 4.23 (2H, t, J=4.2Hz), 4.65-4.75 (1H, m), 5.85 (1H, d, J=14.6Hz), 6.65-6.75 (2H, m), 6.76-6.88 (2H, m), 6.90-7.09 (2H, m), 7.11-7.22 (2H, m) ppm. MS: [M+H]+ = 488.2 Example 20 5-{4-(4-(2-Hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methyIbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-/3][1,4]diazepine (Figure Removed) 20A: 5-(4-Cyano-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-b][1,4]diazepine Thionyl chloride (0.6ml, Q.OOmmol) was added to a suspension of 4-cyano-3-methylbenzoic acid (322mg, 2.00mmol) in toluene (10ml). The mixture was heated at reflux for 2h, allowed to cool and concentrated in vacua. The residue was azeotroped with toluene and then taken up in dichloromethane (5ml). The solution was added slowly to a stirred solution of 1-methyl-4,10-dihydropyrazo!o[4,5-c]pyrido[2,3-/>][1,4]diazepine (400mg, 2.00mmol) and triethylamine (0.35ml, 2.50mmol) in dichloromethane (5ml). The mixture was stirred at room temperature for 24h then concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 5% methanol/chloroform) to give an orange solid identified as 5-(4-cyano-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-6][1,4]diazepine (500mg, 73%). 20B: 5-(4-Arn»nomethyl-3-methylbenzoyl)-1 -methyI-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-6][1,4]diazepine Cobalt(ll) chloride hexahydrate (690mg, 2.90mmol) was added to an ice-cold stirred solution of 5-(4-cyano-3-methylbenzoyl)-1-methyl-4l10-dihydropyrazolo[4l5-c]pyrido[2,3-6][1,4]diazepine (SOOmg, 1.45mmol) in methanol (15ml). Sodium borohydride (570mg, 15.00mmol) was added portionwise and the mixture was stirred at room temperature for 1h. 1M KHSO4 was added, the methanol was removed in vacua, and the aqueous residue was filtered through Celite®. The filtrate was washed with diethyl ether, basified to pH12 with 2M sodium hydroxide and extracted with chloroform. The chloroform extracts were washed with brine and concentrated in vacua to give a pale orange solid identified as 5-(4-aminomethyl-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-i)][1,4]diazepine (400mg, 79%). 20C: 5-(4-(4-(2-Hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-Jb][1,4]diazepine 1,1'-Carbonyldiimidazole (20mg, 0.12mmol) was added to a solution of 5-(4-aminomethyl-3-methylbenzoyl)-1-methyl-4l10-dihydropyrazolo[4,5-c]pyrido[2,3-5][1,4]-diazepine (35mg, O.IOmmol) in DMF (3ml). The solution was stirred for 1h, a solution of 1-(2-hydroxyethyl)piperazine (13mg, O.IOmmol) and DIEA (18^1, O.IOmmol) in DMF (2ml) was added and the mixture was stirred at room temperature for 24h then concentrated in vacua. The residue taken up in chloroform and the solution was washed with brine and concentrated in vacua. The residue was purified by flash chromatography on silica gel (eluant 7% methanol/chloroform) to give a pale yellow solid identified as 5-(4-(4-(2-hydroxyethyl)piperazine-1-carbonylaminomethyl)-3-methylbenzoyl)-1-methyl-4,10-dihydropyrazolo[4,5-c]pyrido[2,3-fa][1,4]diazepine (29mg, 58%). 1H NMR: 6 2.42 (3H, br s), 2.44-2.60 (7H, m), 3.20-3.40 (4H, m), 3.55-3.65 (2H, m), 3.79 (3H, s), 3.85-4.00 (1H, m), 4.26 (2H, brs), 4.88 (1H, br s), 5.80-5.95 (1H, m), 6.60 (1H, br s), 6.80- 7.30 (6H, m), 8.00 (1H, s) ppm. MS: [M+H]* = 505.2 Examples 21-134 The following compounds were prepared using analogous methods to those described Examples 21 - 30 (Figure Removed) 4-(4-Carboxy-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-fa]azepine A suspension of 4-(4-cyano-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-i)]azepine (1g, 3.3mmol) in cone, sulphuric acid/water (1:1, 30ml) was heated at reflux for 5hr. The resulting solution was cooled to RT, diluted with water (20ml) and extracted with chloroform (3 x 20ml). The combined organic phases were extracted with sat. NaHCO3 (2 x 20ml). The combined aqueous extracts were acidified with 1M KHSO4 and extracted with chloroform (3 x 20ml). These chloroform extracts were combined, washed with brine, dried over Na2SO4 and concentrated in vacuo to give a pale brown solid identified as 4-(4-carboxy-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-/)]azepine. (225mg, 23%). 4-(4-Hydroxymethyl-3-methylbenzoyl)-5I6,7,8-tetrahydrothieno[3,2-Jb]azepine Isobutyl chloroformate (250^, 2mmol) was added to a solution of 4-(4-carboxy-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine (470mg, 1.48mmol) and N-methylrnorpholine (230^1, 2.1mmol) in THF (15ml) at 0°C and the mixture was stirred for 1hr. The resultant suspension was filtered and the filtrate was added to a solution of sodium borohydride (131mg, 3.45mmol) in water (15ml) at 0°C. The solution was stirred at RT for 2hr, then sat. NH4CI (5ml) was added and the THF was removed in vacua. The remaining solution was diluted with water and extracted with chloroform (3 x 20ml). The combined organic phases were washed with brine, dried over Na2SO4 and concentrated in vacua to give a pale brown solid identified as 4-(4-hydroxymethyl-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-/)]azepine (330mg, 74%). 4-(4-(1-lmidazolecarbonyloxymethyl)-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine 1,1'-Carbonyldiimidazole (36mg, 0.22mmol) was added to a solution of 4-(4- hydroxymethyl-3-methylbenzoyl)-5A7,8-tetrahydrothieno[3,2-Jb]azepine (60mg, 0.17mmol) in DMF (2ml) under nitrogen gas and the solution was stirred at RT for 18hr. The solvent was removed in vacua and the residue was purified by flash chromatography on silica gel (eluant 97% chloroform/3% methanol) to give a colourless gum identified as 4-(4-(1-imidazolecarbonyloxymethyl)-3-methylbenzoyl)-5,6I7,8-tetrahydrothieno[3,2-Jb]azepine (60mg, 45%). 4-Cyc!opropylmethyl-piperazine-1 -carboxylic acid 2-methyl-4-(5>6,7,8-tetrahydro-thieno[3,2-b]azepine-4-carbonyl)-benzyl ester A mixture of 4-(4-{1-imidazolecarbonyloxymethyl)-3-methylbenzoyl)-5,6,7,8-tetrahydrothieno[3,2-b]azepine (1.0eq), 1-cyclopropylmethyl-piperazine (1.0eq) and DIEA (1.05eg) was heated at reflux for 48h. The mixture was concentrated in vacuo and purified by flash chromatography on silica gel (eluant methanol/chloroform). MS: [M+H]+ = 468 Examples 133 and 134 Prepared by analogous methods. Example 133 (Figure Removed) Example 135 In vitro Testing Compounds were assayed to determine their ability to mimic the cellular consequences of OT stimulation on intact cells. In the assay, the compounds of the invention cause significant cellular activation at concentrations of 30nM or less. Preferred compounds cause significant activation at concentrations of SOOnM or less and can induce the same maximal effect as OT. The preferred compounds are either significantly less active or completely devoid of activity in assays for vasopressin-like activity. Example 136 In vivo Testing Representative compounds were tested for activity in the rat uterine contractility model, which is a recognised test for OT agonism. The compounds increased the strength and frequency of the uterine contractions at doses below 50mg/kg. Selected compounds were then given either i.c.v. or i.v. to male rats and the erectile response was determined. Example 137 Tablet for Oral Administration Tablets containing 100mg of the compound of Example 11 as the active agent are prepared from the following: Compound of Example 11 200.0g Corn starch 71.0g Hydroxypropylcellulose 18.0g Carboxymethylcellulose calcium 13.0g Magnesium stearate 3.0g Lactose 195.0g Total 500. Og The materials are blended and then pressed to give 2000 tablets of 250mg, each containing 100mg of the compound of Example 11. The foregoing demonstrates that the compounds according to the present invention act as agonists at the oxytocin receptor and accordingly they may find utility as pharmaceutical agents for the treatment of conditions such as sexual disorders including male erectile dysfunction, ejaculatory disorders and female sexual dysfunction, cancer of the prostate, breast, ovary and bones, osteoporosis, benign prostatic hyperplasia, post-partum bleeding, and depression. The compounds may also be used to induce labour or delivery of the placenta, to decrease arterial blood pressure, to decrease exaggerated responses to stress and to increase the nociceptive threshold. The scope of the present invention is further defined in the following claims. We claim: 1. A novel benzyl carbamates of general formula 1, or a pharmaceutically acceptable salt or isomers thereof (Formula Removed) wherein: G1 is selected from (Formula Removed) A1 is selected from CH2, CH(OH), NH, N-alkyi, O and S; A2 is selected from CH2, CH(OH), C(=0) and NH; A3 is selected from S. NH, N-alkyl, - CH=CH- and -CH=N-; A4 and A5 are each selected from CH and N; A6 is selected from CH2, NH, N- alkyl and O; A7 and A11 are selected from C and N; A8 and A9 are selected from CH, N. NH, N(CH2)d R7 and S; A10 is selected from -CH=CH-, CH, N. NH, N(CH2) R7 and S; A12 and A13 are selected from N and C; A14, A15 and A16 are selected from NH, N- CH3, S. N and CH; X1 is selected from O and NH; R1, R2 and R3 are each selected from H. alkyl, O-alkyl, F. CI and Br; R4 is selected from H. alkyl, alkenyl, alkynyl, optionally substituted phenyl, optionally substituted thienyl, optionally substituted furyl, optionally substituted pyridyl, (CO)-O-(C H2)eR8, -(CH2)eR8, -CH2-CH=CH- CH2-R8, -CH2-C-C-CH2-R8, -(CH2)g-CH(OH)-(CH2)h-R8, (Formula Removed) R5 and R6 are independently selected from alkyl, Ar and -(CH2)r_Ar; R7 is selected from H. alkyl, optionally substituted phenyl, F. OH, O-alkyl, O-acyi, S- alkyl, NH2, NH-alkyl, N(alkyl)2, NH-acyl, N(aikyl)-acyl, CO2H, C02-alkyl, CONH2l CONH-aikyI, CON(alkyl)2, CN, CF3, optionally substituted pyridyl, optionally substituted thienyl and optionally substituted furyl; R8 is selected from H. alkyl, alkenyl, alkynyl, acyl, optionally substituted phenyl, optionally substituted pyridyl, optionally substituted thienyl, optionally substituted furyl, optionally substituted pyrollyl, optionally substituted pyrazolyl, optionally substituted imidazolyl, optionally substituted oxazolyl, optionally substituted isoxazolyl, optionally substituted thiazolyl, optionally substituted isothiazolyl, F. OH, hydroxyalkyl, O-alkyl, O-acyl, S-alkyl, NH2, NH-alkyl, N(alkyl)2, 1- pyrrolidinyl, 1-piperidinyl, 4-morpholinyi, NH-acyl, N(alkyl)-acyl, N3, C02H, C02-alkyl, CONH2, CONH-alkyI, CON(alkyl)2, ON and CF3; Ar is selected from optionally substituted thienyl and optionally substituted phenyl; a is 1 or 2, b is 1, 2 or 3; c is 1 or 2, d is 1, 2 or 3; e is 1, 2, 3 or4; f is 1, 2 or 3 and g, h, i and j are all independently 1 or 2; provided that: not more than one of A8, A9 and A10 is NH, N(CH2)dR7 or S; A7 and A11 are not both simultaneously N; neither A7 nor A11 is N if one of A8, A9 and A10 is NH, N(CH2)dR7 or S; if A10 is -CH=CH- then A8 is N. A9 is CH and both A7 and A11 are C; if A10 is not -CH=CH- then one of A8, A9 and A'° is NH, N(CH2)dR7 or S or one of A7 and A11 is N; not more than one of A14, A15 and A16 is NH, N-CH3 or S; A12 and A13 are not both simultaneously N; if one of A14, A15 and A16 is NH, N-CH3 or S then A12 and A13 are both C; and one of A14, A15 and A16 is NH, N-CH3 or S or one of A12 and A13 is N. 2. A compound as claimed in claim 1, or a pharmaceutically acceptable salt thereof, wherein at least one of R1, R2 and R3 is H and at least one is not H. 3. A compound as claimed in claim 1 or 2, or a pharmaceutically acceptable salt thereof, wherein one of R1, R2 and R3 is selected from an alkyl group, F. CI and Br and the others are H. 4 .A compound as claimed in any preceding claim, or a pharmaceutically acceptable salt thereof, wherein R' is selected from a methyl group and CI, and R2 and R3 are H. 5. A compound as claimed in any preceding Claim, or a pharmaceutically acceptable salt thereof, wherein X1 is NH. 6 A compound as claimed in any preceding Claim, or a pharmaceutically acceptable salt thereof, wherein a is 1 and b is 2. 7. A compound as claimed in any preceding Claim, or a pharmaceutically acceptable salt thereof, wherein Gil is a group according to general formula 3. 8 .A compound as claimed in claim 7 to or a pharmaceutically acceptable salt thereof, wherein c is 2. 9. A compound as claimed in claim 7 or 8, or a pharmaceutically acceptable salt thereof, wherein A1 is CH2and A2 is NH. 10. A compound as claimed in claim 7 or 8, or a pharmaceutically acceptable salt thereof, wherein A1 is NH or N-alkyl and A2 is C(=0). 11. A compound as claimed in any of claims Claims 7 to 10, or a pharmaceutically acceptable salt thereof, wherein A3 is S and A4 and A5 are both CH. 12. A compound as claimed in any of Claims 7 to 10, or a pharmaceutically acceptable salt thereof, wherein A3 is -CH=CH- and A4 and A5 are both CH. 13. A compound as claimed in any of Claims 7 to 10, or a pharmaceutically acceptable salt thereof, wherein A3 is -CH=N- and A4 and A5 are both CH. 14. A compound as claimed in any of Claims 7 to 10, or a pharmaceutical^ acceptable salt thereof, wherein A3 is -CH=CH-, A4 is CH and A5 is N. 15. A compound as claimed in any of Claims 1 to 6, or a pharmaceutical^ acceptable salt thereof, wherein G1 is a group according to general formula 6 or 7 16. A compound as claimed in claim 15 or a pharmaceutically acceptable salt thereof, wherein A3 is S and A4 and A5 are both CH. 17. A compound as claimed in claim 15, or a pharmaceutically acceptable salt thereof, wherein A3 is -CH=CH- and A4 and A5 are both CH. 18. A compound as claimed in claim 15, or a pharmaceutically acceptable salt thereof, wherein A3 is -CH=N- and A4 and A5 are both CH. 19. A compound as claimed in claim 15, or a pharmaceutically acceptable salt thereof, wherein A3 is -CH=CH-, A4 is CH and A5 is N. 20. A compound as claimed in any of Claims 1 to 6, or a pharmaceutically acceptable salt thereof, wherein G1 is a group according to general formula 4 or 6 21. A compound as claimed in claim 20, or a pharmaceutically acceptable salt thereof, wherein A6 is NH. 22. A compound as claimed in claim 20 or 21, or a pharmaceutically acceptable salt thereof, wherein A5 is NH or N-(CH2)d-R7. 23. A compound as claimed in claim 22, or a pharmaceutically acceptable salt thereof, wherein A9 is N and A10 is CH. 24. A compound as claimed in claim 1, or a pharmaceutically acceptable salt thereof, wherein R1 is methyl or CI, R2 and R3 are both H and X1 is NH. 25. A compound as claimed in claim 1 or 24, or a pharmaceutically acceptable salt thereof, wherein R1 is methyl or CI, R2 and R3 are both H. X1 is NH, a is 1 and b is 2. 26 .A compound as claimed in claim 1, or a pharmaceutically acceptable salt thereof, wherein G1 is a group according to general formula 6, A4, A5 and A10 are all CH, A6 is NH, A7 and A11 are both C, A8 is N-(CH2)d-R7 and A9 is N. 27. A compound as claimed in claim 1, or a pharmaceutically acceptable salt thereof, wherein R1 is methyl or CI, R2 and R3 are both H. X1 is NH, a is 1, b is 2, G1 is a group according to general formula 6, A4, A5 and A10 are all CH, A6 is NH, A7 and A11 are both C, A8 is N-(CH2)d-R7 and A9 is N. 28. A compound as claimed in claim 1 selected from 5-(4-(4- cyclopropylmethylpiperazine-1 -carbonylaminomethyl)-3-methylbenzoyl)-1 - methyl-4, 1 0-dihydropyrazolo[5,4-b][1,5] benzodiazepine, 5-(4-(4- benzylpiperazine-1 -carbonylaminomethyl)-3- methylbenzoyl)-1 -methyl-4 10-dihydropyrazolo[5,4-b][1, 5];benzodiazepine, 5-(4-(4-(3-hydroxybenzyl) piperazine-1 - carbonylaminomethyl)-3-methylbenzoyl)-1 - methyl-4 1 0-dihydropyrazolo[5,4-b][1, 5]benzodiazepine, 5-(4-(4- (3- hydroxymethylbenzyl)piperazine-1 -carbonylaminomethyl)-3- methylbenzoyl)- 1 -methyl-4, 1 0-dihydropyrazolo[5,4-b][1, 5]benzodiazepine, 1 -methyl-5- (3-methyl-4-(4-(4-picolyl)piperazine- 1 -carbonylaminomethyl)benzoyl)-4, 10-dihydropyrazolo[5,4-b][1,5]benzodiazepine, 5-(4-(4-(2-hydroxyethyl) piperazine-1 - carbonylaminomethyl)-3-methylbenzoyl)-1 - methyl-4, 1 0-dihydropyrazolo[5,4-b][1,5]benzodiazepine, 1 -methyl- 5-(3- methyl-4-(4-(3-(methylthio)propyl)piperazine-1 - carbonylaminomethyl)benzoyl)-4, 1 0-dihydropyrazolo[5,4-b][1,5]benzodiazepine, 5-(4-(4-(2-aminoethyl)piperazine-1 - carbonylaminomethyl)-3-methylbenzoyl)- 1 -methyl- 4,1 0-dihydropyrazolo[5,4-b][1,5];benzodiazepine, 5-(4-(4-(2- hydroxyethyl) piperazine-1 -carbonylaminomethyl)-3-methylbenzoyi)-1 - methyl-4, 1 0-dihydropyrazolo[4,5-c][2,3-b][1,4]diazepine, and pharmaceutically acceptable salts thereof. 29 A pharmaceutical composition as claimed in any preceding claim as and when used in the preparation of medicament for the treatment of male erectile dysfunction. |
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00211-delnp-2004-complete specification (granted).pdf
00211-delnp-2004-correspondence-others.pdf
00211-delnp-2004-description (complete)-02-01-2009.pdf
00211-delnp-2004-description (complete)-03-09-2008.pdf
00211-delnp-2004-description (complete).pdf
00211-DELNP-2004-Form-2-(02-01-2009).pdf
00211-delnp-2004-petition-138.pdf
0211-DELNP-2004-Claims-(02-01-2009).pdf
211-DELNP-2004-Abstract-(03-09-2008).pdf
211-DELNP-2004-Abstract-(12-09-2008).pdf
211-DELNP-2004-Claims-(03-09-2008).pdf
211-DELNP-2004-Claims-(12-09-2008).pdf
211-DELNP-2004-Correspondence-Others-(03-09-2008).pdf
211-DELNP-2004-Correspondence-Others-(07-01-2009).pdf
211-DELNP-2004-Correspondence-Others-(08-09-2008).pdf
211-DELNP-2004-Correspondence-Others-(12-09-2008).pdf
211-DELNP-2004-Form-1-(07-01-2009).pdf
211-DELNP-2004-Form-1-(12-09-2008).pdf
211-DELNP-2004-Form-2-(07-01-2009).pdf
211-DELNP-2004-Form-2-(12-09-2008).pdf
211-DELNP-2004-Form-3-(03-09-2008).pdf
211-DELNP-2004-Form-3-(08-09-2008).pdf
| Patent Number | 230572 | ||||||||
|---|---|---|---|---|---|---|---|---|---|
| Indian Patent Application Number | 00211/DELNP/2004 | ||||||||
| PG Journal Number | 11/2009 | ||||||||
| Publication Date | 13-Mar-2009 | ||||||||
| Grant Date | 27-Feb-2009 | ||||||||
| Date of Filing | 29-Jan-2004 | ||||||||
| Name of Patentee | See attached documents | ||||||||
| Applicant Address | See attached documents | ||||||||
Inventors:
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| PCT International Classification Number | C07D 495/04 | ||||||||
| PCT International Application Number | PCT/GB02/03593 | ||||||||
| PCT International Filing date | 2002-08-06 | ||||||||
PCT Conventions:
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