Title of Invention | "METHOD FOR PREPARING PHENYLETHANOLAMINES COMPOUNDS AND PHARMACEUTICALLY ACCEPTABLE SALTS THEREOF" |
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Abstract | The invention relates to method for preparing compounds of formula (I). The compounds of the present invention have the effect of ß2-receptor agonist and can be sued for the treatment of asthma and bronchitis. The compounds of formula (I) are prepared by the reaction of compounds of formula (III) and the compounds of fonnula (IV) in the anhydrous condition, in a reacting solvent of alcohols or aromatic hydrocarbons. The reacting temperature is refluxing temperature of: solvent, the reacting period is 10-15h. |
Full Text | Technical Field The present invention relates to new compounds for the treatment of asthma and bronchitis, in particularly, new phenylethanol- amines compounds asß- receptor agonist. Background Art The asthma and bronchitis are common diseases. In most case, their therapies are through using antibiotics, which are not very effective and have some side effect in longer usages-Receptor agonists are well known as anti-asthma agents. However, these agents are still deficient in effects and physical and chemical properties. Disclosure of the invention The invention relates to phenylethanol-amines compounds of formula (D) and pharmaceutically acceptable salts thereof: (Figure removed) wherein RI is H, chlorine, or bromine; R2 is electron attractive groups selected from the group consisting of CF3, CN, fluorine, CH3SO3, CF3SO3, andNO2; R3 is linear or branched alkyl having 1 to 10 carbon atoms, linear or branched alkoxyalkyl having 2 to 10 carbon atoms, aliphatic alcohol having 1 to 10 carbon atoms, or cycloalkyl having 3 to 6 carbon atoms. According to one embodiment of the invention, R2 is preferably CF3 or CN. According to another embodiment of the invention, R3 is linear or branched alkyl having 1 to 6 carbon atoms, linear or branched alkoxy having 2 to 6 carbon atoms, aliphatic alcohol having 1 to 6 carbon atoms, or cycloalkyl having 3 to 6 carbon atoms. The term "pharmaceutically acceptable salt" used in herein refers to conventional acid-addition salts or base-addition salts which retain the biological effectiveness and properties of the compounds of formula (D) and are formed from suitable non-toxic organic or inorganic acids or organic or inorganic bases. Sample acid-addition salts include those derived from inorganic acids such as hydrochloric acid, hydrobromic acid, hydroiodic acid, sulfuric acid, phosphoric acid and nitric acid, those derived from organic acids such as acetic acid, tartaric acid, salicylic acid, methanelsulfonic acid, butanedioic acid, citric acid, malic acid, lactic acid, fumaric acid, and the like. Sample base-addition salts include those derived from potassium, sodium, ammonium. In particularly, the pharmaceutically acceptable salts of the compounds of formula (D) are preferably hydrochloride or hydrobromide. The present invention also provides a method for preparing the compounds of formula (D), comprising reacting the free base of formula (D) or pharmaceutically acceptable salts thereof (Figure removed) wherein RI and R2 are as defined above, with the compounds of formula ( D ) H2NR3DDD wherein Ra is as defined above. The compounds of formula (D) according to the present invention can be prepared by the above methods. The reaction of compounds of formula (D) and the compounds of formula (D) is carried out in the anhydrous condition, for example in the solvent of alcohols, such as anhydrous ethanol or aromatic hydrocarbons, such as toluene at a temperature of refluxing temperature of solvent for 10-15h. The yield is 20-30%. In the present invention, compounds of formula (D) can be prepared by the following scheme: (Figure removed) wherein the p-amino acetophenone can be used as free base of formula (D) or pharmaceutically acceptable salts thereof. The method for preparing compounds of formula (D) from compounds of formula (D) is well known to those skilled in the art ( for example, Kurger G, Keck J. and Pieper H. Synthesis of amino-Halogen-Substituted Phenyl-aminoethanols. Arzneim Forsch./Drug res. 34(1 1), Nr. Ba, 1984:1612-1624, which is incorporated herein by reference). The compounds of formula (D) are prepared from the compounds of formula (D) by reduction with potassium borohydride in methanol and water at room temperature for 5h. The present invention also provides a pharmaceutical composition comprising at least one compound of formula (D) or pharmaceutically acceptable salts thereof. The pharmaceutical composition according to the present invention further comprises one or more pharmaceutically acceptable excipients and other active ingredients. The "pharmaceutically acceptable excipients" means an excipient that is useful in pharmaceutical fields that is generally safe, non-toxic and neither biologically nor undesirable effect. These excipients also include lactose, starch, water, alcohol, and the like. The pharmaceutical composition according to the present invention can also include propellents, antiseptics, solubilizing agents, stabilizing agents, moistening agents, emulsifiers, sweeting agents, colorants, flavoring agents, salts for adjusting osmotic pressure, buffer, coating agents, antioxitants, and the like. The pharmaceutical composition according to the present invention can also comprise other therapeutically valuable substance, for example other active ingredients other than the compound of formula (D). The pharmaceutical composition according to the present invention can be prepared into tablets, capsules, solutions, sprays, injections, and the like. It can be administrated by oral, parenteral, spraying, inhaling through oral or nasal cavity or other forms. The compounds of the present invention have the effect of ß2- receptor agonist and can be used for the treatment of asthma and bronchitis. The present invention relates to use of the compound of formula (D) in the preparation of medicaments having effect of fo-receptor agonist. The present invention also relates to use of the compound of formula (D) in the preparation of medicaments for the treatment of asthma and bronchitis. The compounds of the present invention can be administrated in a therapeutically effective amount. The "a therapeutically effective amount" means an amount that effectively prevent, alleviate, improve the diseases conditions. The "a therapeutically effective amount" can be determined by those skilled in the art. The therapeutically effective amount or dose may be changed in a broad scope, and may be adjusted according to requirement of individual case. Typically, for adults with about 70Kg weight, preferably the dose is about 50|Jg-10 mg /day when administrated in oral or parenteral form. When required, the upper limit and low limit of dose can be exceeded. The daily dose can be administrated alone or divided in several times. The compounds according to the present invention can be prepared according to above scheme by using known synthesis methods. The following examples illustrate preferable synthesis method of these compounds. EXAMPLE 1 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylamino-ethanol hydrochloride a. Preparation of 4-amino-3-chloro-5-trifluoromethyl-benzoyl chloride 13g (0.0543mol) of 4-amino-3-chloro-5-trifluoromethyl-benzoic acid was added to 32.5ml of thionyl chloride. The suspension was heated until the crystals have dissolved, then refluxing was continued for another 2h. After cooling to room temperature, the remaining thionyl chloride was evaporated under reduced pressure, thus obtained crude 3-chloro-4-amino-5-trifluoromethyl-benzoyl chloride, which was dissolved in chloroform at heating. Filtered with heating and evaporated under reduced pressure to remove chloroform, obtained the subject product. Yield: 80-90%, melting point: 110-115°C. b. 4-amino-3-chloro-5-trifluoromethyl-acetophenone To reaction flask 1.3 Ig (0.0535mol) of magnesium turnings, 1.6ml of absolute ethanol and 0.12ml of carbon tetrachloride were added at room temperature. Heated, 14.6ml of absolute tetrahydrofuran were added at such a rate that refluxing was maintained. Under continued refluxing and stirring a mixture of 8.1ml(0.0534mol) of diethyl malonate, 4.8ml of absolute ethanol and 5.6ml of tetrahydrofuran was added dropwise over Ih, followed by reflux for 2h. 13.1g (0.05 Imol) 4-amino-3-chloro-5-trifluoromethyl-benzoyl chloride was dissolved in 43.5ml tetrahydrofuran, and was added dropwise to above reaction solution over 0.5h. After added, continue to reflux for 2h. After cooling to room temperature, 2N sulfuric acid were dropped to adjust pH to 2. Organic phase was separated, evaporated under reduced pressure to obtain oil. A mixture of 45.8ml of glacial acetic acid, 30.6ml of water and 5.7ml of concentrated sulfuric acid was added, refluxed with heating for 5h. Evaporated under reduced pressure to remove solvent. The solid obtained was dissolved in chloroform. Ice water was added, and pH was adjusted to 8 with 50% solution of sodium hydroxide. The chloroform phase was separated, washed with water, dried, filtered, and evaporated under reduced pressure to remove chloroform. The crude was obtained. Yield: 75-85%, melting point: 120-130°C. c. 4-amino-3-chloro-5-trifluoromethyl-alpha-bromo- acetophenone 8.5g (0.0358mol) of 4-amino-3-ch'loro-5-trifluoromethyl-acetophenone was dissolved in 85ml of glacial acetic acid. At 45-50°C a solution of 2ml (0.0394mol) of bromine in 17ml of glacial acetic acid was added dropwise. Heating was continued for a further 30 min. The acetic acid was evaporated, the oily residue was taken up in 100ml of ethyl acetate, washed with sodium hydrogen carbonate solution and water respectively, dried and evaporated under reduced pressure to obtain crude product, which was recrystallized in mixed solvents of toluene and cyclohexane to obtained purified crystals. Yield 50-60%;melting point 113-115'C. d. 5.6g (0.01769mol) 4-amino-3-chloro-5-trifluoromethyl-alpha-bromo- acetophenone was dissolved in 56ml of methanol and 4.9ml of water was added. At room temperature 0.96g (0.1769mol) of potassium borohydride were added in small portions and the reaction mixture was stirred for 5h, then cooled to ffC with ice-water and carefully acidified to a pH=2 with 2N hydrochloric acid. Evaporated under reduced pressure and the remaining mass was dissolved in 11.2ml of water and extracted with chloroform (3x 10ml). The organic phase was washed with water to neutrality, dried over anhydrous MgSCU and evaporated to dryness, to give (4-amino-3-chloro-5-trifluoromethyl-phenyl)-ethylene oxide as oil. Yield 85-95%; 'H-NMR (DMSO-^j) 8D2.88(2Hnd)n3.89(lHnt)D7.08(lHDs)D7.24 DIHDs). e. 5.2g (0.022mol) of (4-amino-3-chloro-5-trifluoromethyl-phenyl)-ethylene oxide was dissolved in 26ml of anhydrous ethanol and treated with 5.1ml (0.049mol) of tert-butylamine. The mixture was refluxed for 13h, and then evaporated. The residue was extracted with 2N hydrochloric acid for several times. Aqueous layers were combined and extracted with toluene and treated with activated carbon. The pH was adjusted to 10 with 20% sodium hydroxide solution. The precipitate was collected by filtration, 2-(4-amino-3-chloro-5-trifluoromethylphenyl)-2-tert-butylaminoethanol was obtained. Yield 20-30%; melting point 85-90°C. f. 1. Og of 2-(4-amino-3 -chloro-5 -trifluoromethylphenyl)-2-tert-butylaminoethanol was dissolved in 20ml of diethyl ether and filtered. Saturated solution of hydrogen chloride in isopropanol was added dropwise and acidified to pH=2. The precipitate was collected by filtration, washed with anhydrous ether, and dried to give crude 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylaminoethanol hydrochloride. The crude product was dissolved in absolute ethanol at a ratio of 1:5 w/v. Filtered, anhydrous ether was added dropwise until small amount of crystals was precipitated. Lyophilized and filtered to give 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylaminoethanol hydrochloride. Yield 80-90%; melting point 205-206 °C (dec). 'H-NMR (DMSO-dg) 8:1.24 (9H,s), 3.77(2H,d), 4.42-4.44(lH,m), 7.72(lH,s), 7.87(lH,s). EXAMPLE 2 a. Preparation of 3-iodo-4-amino-acetophenone 40g of 4-aminoacetophenone, 150g of iodine and 59.4g of calcium carbonate were dissolved in 1.2 L methanol and 230mL water and stirred at room temperature for 70-80 h. Sodium thiosulfate was added, stirred, filtered, and evaporated. Aqueous layer was extracted with chloroform and washed with sodium thiosulfate and water in turn. Evaporated to give product as red brown oil. Yield 60-90%. b. Preparation of 3-cyano-4-amino-acetophenone The 3-iodo-4-amino-acetophenone as prepared above was dissolved 95ml of DMF and 20.9g CuCN was added. Stirred under reflux for 6h and cooled down to 100"C. The reaction mixture was poured into 2L of water, and cooled. The precipitate was filtered off, air dried and extracted with THF. Evaporated, washed with ethanol, filtered, and dried to give product as yellow crystal. Yield 56.9%; melting point 150-152°C. c. Preparation of 3-cyano-4-amino-alpha-bromo-acetophenone The mixture of 20.0g of 3-cyano-4-amino-acetophenone and 54.28g of copper bromide in 300ml of THF was refluxed for 4h, cooled, and filtered at room temperature. The filtrate was distilled in vacuo to remove THF. The residue was washed with small amount of ethanol to give title product as yellow solid. Yield 94.8%; melting point 160-161 °C.(decomp.). d. Preparation of 3-cyano-4-amino-5-bromo-acetophenone 2.0g of 3-cyano-4-amino-alpha-bromo-acetophenone was dissolved in 40ml of glacial acetic acid. Stirred and heated to 35°C. 1.48g of NBS was added to the solution in small portions and continue to stir for Ih at the same temperature, then poured into 120mL of water. The precipitate was filtered off and dried to give title product as yellow solid. Yield 82.8%; melting point 165-167C EXAMPLES 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-isopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-d6D δ□1.08(6H,d),2.84-2.86(lH,m), 3.80(2H,d), 4.37-4.39(lH,m), 7.70 (lH,s), 7.80(lH,s). EXAMPLE 4 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-cyclopentylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-d6□δ□ 1.62-1.64□4H,m□, 1.65-1.69(4H,m), 2.64-2.68(lH,m), 3.79(2H,d), 4.43-4.46(lH,m), 7.62(lH,s), 7.77(lH,s).EXAMPLES 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-cyclohexylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-d6□ δ□ 1.29-1.31 □6H,m□, 1.40-1.44(4H,m), 2.78-2.81(lH,m), 3.74(2H,d), 4.39-4.41(lH,m), 7.62(lH,s), 7.89(lH,s). EXAMPLE 6 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-tert-butylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-d6□ δ □ 1.25(9H,s), 3.76(2H,d), 4.40-4.42(lH,m), 7.62(lH,s), 7.78(lH,s). EXAMPLE 7 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-isopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6 □ δ□1.08(6H,d),2.83-2.86(lH,m), 3.82(2H,d), 4.32-4.34(lH,m), 7.76 (lH,s), 7.90(lH,s). EXAMPLE 8 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-cyclopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR □ DMSO-d6 □ δ □ 0.80-0.86(4H,m), 1.60-1.63(lH,m), 3.82(2H,d), 4.40-4.42(1 H,m), 7.69(lH,s), 7.88(lH,s). EXAMPLE 9 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-cyclobutylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR □ DMSO-d6 □δ □ 2.00-2.05(2H,m), 2.14-2.18(4H,m), 3.13-3.16(lH,m), 3.79(2H,d), 4.40-4.42(lH,m), 7.68(lH,s), 7.78(lH,s). EXAMPLE 10 2-(4-amino-3-chloro-5-cyanophenyl)-2-tert-butylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR □ DMSO-D6 δ □1.26(9H,s), 3.75(2H,d), 4.39-4.41(lH,m), 7.79(lH,s), 7.92(lH,s). EXAMPLE 11 2-(4-amino-3-chloro-5-cyanophenyl)-2-isopropylaraino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMP□DMSO-d6 δ□l.08(6H,d),2.82-2.86(lH,m), 3.78(2H,d), 4.38-4.40(lH,m), 7.75(lH,s),7.89(lH,s). EXAMPLE 12 2-(4-amino-3-chloro-5-cyanophenyl)-2-cyclobutylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR D DMSO-d6 □ δ □ 2.05-2.07(2H,m), 2.11-2.16(4H,m), 3.10-3.13(lH,m), 3.77(2H,d), 4.41-4.43(lH,m),7.78(lH,s), 7.88(lH,s). EXAMPLE 13 2-(4-amino-3-chloro-5-cyanophenyl)-2-cyclopentylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-D6 □ δ□1.62-1.65□4H,mn, 1.67-1.69(4H,m), 2.53-2.57(lH,m), 3.75(2H,d), 4.44-4.46(lH,m), 7.72(lH,s), 7.97(lH,s). EXAMPLE 14 2-(4-amino-3 -bromo-5-cyanophenyl)-2-tert-butylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6 □ δ□1.24(9H,s), 3.72(2H,d), 4.36-4.38(lH,m), 7.75(lH,s), 7.95(lH,s). EXAMPLE 15 2-(4-amino-3-bromo-5-cyanophenyl)-2-isopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-d6□ δ□1.06(6H,d), 2.84-2.87(lH,m), 3.75(2H,d), 4.40-4.43(lH,m), 7.79 (lH,s), 7.89(lH,s). EXAMPLE 16 2-(4-amino-3-bromo-5-cyanophenyl)-2-cyclobutylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□2.10-2.13(2H,m), 2.14-2.17(4H,m), 3.13-3.16(lH,m), 3.76(2H,d), 4.40-4.43(lH,m), 7.78(lH,s), 7.92(lH,s). EXAMPLE 17 2-(4-amino-3-bromo-5-cyanophenyl)-2-cyclopentylamino-ethanol hydrochloride was prepared in a method analogous to Example 1 . 1H-NMR□DMSO-d6□ δ□1.60-1.63□4H,m□, 1.65-1.68(4H,m), 2.51-2.53(lH,m), 3.73(2H,d), 4.42-4.45(lH,m), 7.78(lH,s), 7.87(lH,s). EXAMPLE 18 2-(4-amino-3-bromo-5-cyanophenyl)-2-cyclohexylamino-ethanol hydrochloride was prepared in a method analogous to Example 1 . 1H-NMR□DMSO-d6□ δ□1.30-1.35□6H,m□, 1.45-1.49(4H,m), 2.80-2.86(lH,m), 3.76(2H,d), 4.38-4.43(lH,m), 7.76(lH,s), 7.89(lH,s). EXAMPLE 19 2-(4-amino-3-cyano-phenyl)-2-tert-butylamino-ethanol hydrochloride was prepared in a method analogous to Example 1 . 1H-NMR□DMSO-d6 δ□1.25(9H,s), 3.72(2H,d), 4.41-4.42(lH,m), 7.62□lH,d□, 7.70(lH,s), 7.85(lH,d). EXAMPLE 20 2-(4-amino-3-cyano-phenyl)-2-isopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1 . 1H-NMR□DMSO-d6□ δ□1.08(6H,d),2.77-2.79(lH,m), 3.79(2H,d), 4.43-4.46(lH,m), 7.69 (lH,d), 7.72(lH)s),7.80(lH,d). EXAMPLE 21 2-(4-amino-3-cyano-phenyl)-2-cyclobutylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR □ DMSO-D6□δ□ 2.09-2.1 l(2H,m), 2.13-2.19(4H,m), 3.18-3 .21(lH,m), 3.75(2H,d), 4.38-4.3 l(lH,m), 7.68(lH,d), 7.75(lH,s), 7.82(lH,d). EXAMPLE 22 2-(4-amino-3-cyano-phenyl)-2-cyclopentylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□1.62-1.65□4H,m□, 1.68-1.72(4H,m), 2.53-2.56(lH,m), 3.70(2H,d), 4.48-4.5 l(lH,m), 7.68(lH,d), 7.73(lH,s), 7.87(lH,d). EXAMPLE 23 2-(4-amino-3 -cyano-phenyl)-2-cyclopropylamino-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR □ DMSO-D6 □ δ□ 0.89-0.93(4H,m), 1.23-1.26(lH,m), 3.75(2H,d), 4.38-4.42(lH,m), 7.69(lH,d), 7.76(lH,s), 7.80(lH,d). EXAMPLE 24 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-(2-methyl-3-hydroxyl-2-propylami no)-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□1.18(6H,s), 3.61(2H,s), 3.94(2H,d), 4.20-4.23(lH,m), 6.95(lH,s),7.11(lH,s). EXAMPLE 25 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-(2-methyl-3-hydroxyl-2-propylami no)-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6 □ δ□ 1.18(6H,s), 3.68(2H,s), 3.94(2H,d), 4.18-4.21(lH,m), 7.06(lH,s), 7.08(lH,s). EXAMPLE 26 2-(4-amino-3 -chloro-5 -cyanopheny l)-2-(2-methyl-3 -hydroxyl-2-propylamino)-ethan ol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□ 1.17(6H,s), 3.62(2H,s), 4.01(2H,d), 4.16-4.18(lH,m), 7.09(lH,s), 7.20(lH,s). EXAMPLE 27 2-(4-amino-3-bromo-5-cyanophenyl)-2-(2-methyl-3-hydroxyl-2-propylamino)-ethan ol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□ 1.l9(6H)s), 3.60(2H,s), 3.98(2H,d), 4.06-4.09(lH,m), 7.09(lH,s), 7.32(lH,s). EXAMPLE 28 2-(4-amino-3-cyano-phenyl)-2-(2-methyl-3-hydroxyl-2-propylamino)-ethanol hydrochloride was prepared in a method analogous to Example 1. 1H-NMR□DMSO-d6□ δ□1.20(6H,s), 3.56(2H,s), 3.98(2H,d), 4.10-4. 6.60(lH,d), 7.13(lH,s),7.20(lH,d). EXAMPLE 29 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylamino-ethanol lydrobromide 1 .0g of 2-(3-chloro-4-amino-5-trifluoromethyl-phenyl)-2-tert-butylaminoethanol was dissolved in 20ml of anhydrous diethyl ether and the solution was acidified to pH=2 by adding dropwise a solution of hydrobromic acid in isopropanol with stirring. The precipitate was collected by filtration, washed with small amount of anhydrous diethyl ether, dried to give crude 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylamino-ethanol hydrobromide. The crude product was dissolved in absolute ethanol at a ratio of 1:5 w/v. Filtered and anhydrous diethyl ether was added dropwise until small amount of crystals was precipitated. Lyophilized and filtered to give 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-tert-butylamino-ethanol hydrobromide. Yield 80-90%; melting point 208-210°C (dec). 1H-NMR □ DMSO-d6□ δ□ 1.24(9H,s), 3.79(2H,d), 4.46-4.5l(lH,m), 7.72(lH,s), 7.89(lH,s). EXAMPLE 30 2-(4-amino-3-chloro-5-trifluoromethyl-phenyl)-2-(3-ethoxyl-2-propylamino)-ethanol hydrochloride was prepared in a method analogous to Example 1. 'H-NMR□DMSO-D6□ δ:1.08D3H,tO,1.84-1.98(2H,m), 2.71-2.84(2H,m), 3.32-3.39(4H,m), 3.82(2H,d), 4.25-4.27(lH,m),5.60(lH,s), 5.90(2H,s), 7.69(lH,s), 7.87(lH,s), 9.39(2H,s). EXAMPLE 31 2-(4-amino-3-bromo-5-trifluoromethyl-phenyl)-2-(3-ethoxyl-2-propylamino)-ethanol hydrochloride was prepared in a method analogous to Example 1. !H-NMR D bMSO-^j D 5 :1.09 D 3H,t D ,1.92-1.98(2H,m), 2.73-2.78(2H,m), 3.30-3.36(4H,m), 3.79(2H,d), 4.22-4.26(lH,m),5.68(lH,s), 5S9(2H,s), 7.71(lH,s), 7.86(lH,s), 938(2H,s). Experiment example The antagonistic effects of bronchoconstrtriction induced by histamine of the compounds of the present invention were evaluated by isolated guinea pig trachea strips. Apparatus: polygrapher recorder, strain gauge transducer Conditions: Krebs-Hensleit solution; gas mixture(95DO2, 5DCO2); Paper speed: 4mm/min; 37°C Animals: guinea pigs (Harley, purchased from the Experimental Animal Center of China Medical Univesity) of either sex weighting 350-500 g were used. Reagent: Histmaine phosphate solution(10"6D 10"4M) Sample: Depending on their potencies, the compounds were tested at the concentration of 1 0"6 or 3 X 1 0"4M. Method: Guinea pigs were sacrificed and the trachea strips(2cmx 3mm) were prepared; the preparation was then mounted under a testing tension of 2g in an organ bath containing 10 mL Kebs-Hensleits solution at 3TC and supervised with the gas mixture mentioned above and the preparation was allowed to equilibrate for 2 h before the addition of histamine. When the tension of trachea strips reached 50 % of the maximum contraction, the tested compounds was added to bath, and the antagonistic effect (represented as relaxing rate) was calculated as below: Relaxing rate = (Contraction intensity after histamine addition-Contraction intensity after tested compounds addition)/ Contraction intensity after tested compounds addition X 100D The relaxing rate of each compound was presented in table 1. (Table Removed) The above results showed that the compounds of the present invention have an alleviation effect on trachea spasm induced by histamine. 1. Compounds of formula (D) (Formula Removed) wherein: RI is H, chlorine, or bromine; R2 is electron attractive groups selected from the group consisting of CF3, CN, fluorine, COS03H, CF3SO3, andNO2; RS is linear or branched alkyl having 1 to 10 carbon atoms, linear or branched alkoxyalkyl having 2 to 10 carbon atoms, aliphatic alcohol having 1 to 10 carbon atoms, or cycloalkyl having 3 to 6 carbon atoms; and pharmaceutically acceptable salts thereof. 2. The compound according to Claim 1, wherein R2 is CF3 or CN. 3. The compound according to Claim 1, wherein R3 is linear or branched alkyl having 1 to 6 carbon atoms, linear or branched alkoxy having 2 to 6 carbon atoms, aliphatic alcohol having 1 to 6 carbon atoms, or cycloalkyl having 3 to 6 carbon atoms. 4. The compound according to Claim 1, wherein the pharmaceutically acceptable salts of the compounds of formula (D) are hydrpchloride or hydrobromide. 5. A method for preparing the compounds of Claim 1, comprising reacting the free alkali of formula (D) or pharmaceutically acceptable salts thereof (Figure Removed) wherein RI and R2 are as defined above, with the compounds of formula (D) H2NR3nn wherein R3 is as defined above. 6. The method according to Claim 5, wherein the reaction of compounds of formula (D) and the compounds of formula (D) is carried out in the anhydrous condition, the reacting solvent is alcohols or aromatic hydrocarbons, the reacting temperature is refluxing temperature of solvent, the reacting period is 10-15h, and the yield is 20-30%. 7. A pharmaceutical composition comprising the compounds according to any one of claims 1-4 and pharmaceutically acceptable excipients. 8. Use of the compound according to any one of claims 1-4 in the preparation of medicaments having effect of ß2- receptor agonist. 9. Use of the compound according to any one of claims 1-4 in the preparation of medicaments for the treatment of asthma and bronchitis. 10. Compound of formula (), substantially as hereinbefore described with reference to the foregoing examples. 11. A method for preparing the compound of formula (), substantially as hereinbefore described with reference to the foregoing examples. 12. A pharmaceutical composition, substantially as hereinbefore described with reference to the foregoing examples. 13. Use of the compound of formula (), substantially as hereinbefore described with reference to the foregoing examples. |
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745-delnp-2004-correspondence-others.pdf
745-delnp-2004-correspondence-po.pdf
745-delnp-2004-description (complete).pdf
745-delnp-2004-petition-138.pdf
Patent Number | 226575 | ||||||||||||||||||||||||
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Indian Patent Application Number | 745/DELNP/2004 | ||||||||||||||||||||||||
PG Journal Number | 01/2009 | ||||||||||||||||||||||||
Publication Date | 02-Jan-2009 | ||||||||||||||||||||||||
Grant Date | 19-Dec-2008 | ||||||||||||||||||||||||
Date of Filing | 23-Mar-2004 | ||||||||||||||||||||||||
Name of Patentee | JINZHOU JIUTAI PHARMACEUTICAL CO. LTD. | ||||||||||||||||||||||||
Applicant Address | NO. 41, TAIANLI, TAIHE DISTRICT, JINZHOU, LIAONING 121021 P.R.CHINA. | ||||||||||||||||||||||||
Inventors:
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PCT International Classification Number | C07C 215/28 | ||||||||||||||||||||||||
PCT International Application Number | PCT/CN02/00676 | ||||||||||||||||||||||||
PCT International Filing date | 2002-09-25 | ||||||||||||||||||||||||
PCT Conventions:
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