CN1279238A - Process for preparing sypolyphenol - Google Patents
Process for preparing sypolyphenol Download PDFInfo
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- CN1279238A CN1279238A CN 99109345 CN99109345A CN1279238A CN 1279238 A CN1279238 A CN 1279238A CN 99109345 CN99109345 CN 99109345 CN 99109345 A CN99109345 A CN 99109345A CN 1279238 A CN1279238 A CN 1279238A
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- propyl
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Abstract
A process for preparing sypolyphenol includes such steps as reacting of difluorobenzoyl chloride on 1-methyl-4-nitro-3-n-propylpyrazole-5-formamide to obtain 5-(2-flocorophenyl)-1-methyl-3-n-propyl-1,6-dihydrogen-7-H-pyrazol[4.3-d] pyrimidine-7-ketone, linking it with piperazinyl, and substituting fluorine with ethoxy.
Description
The present invention relates to a kind of preparation method of impotence treatment medicine ' Xiduofeng '.
'Xiduofeng ' is a kind of medicine for the treatment of impotence of Pfizer Inc.'s nineteen ninety invention, worldwide listing in 1998.
Chinese patent 91104162 discloses a kind of preparation method of 'Xiduofeng '; this method is carried out sulfonylation by piperazine group and 5-phenyl-pyrazolopyrimidine main body and is realized being connected of two groups, is wherein replaced by alkoxyl group on 2 of 5-phenyl in 5-phenyl-pyrazolopyrimidine main body.
Chinese patent 94192386 discloses the application of the treatment impotence of 'Xiduofeng '.
Chinese patent 97113261 discloses by the ring-closure reaction to pyrimidone part in the 'Xiduofeng ' structure, this ring-closure reaction the piperazine group with carry out after benzenesulfonyl is connected.
Investigator of the present invention has worked out a kind of synthetic method different with above-mentioned synthetic method, the preparation method of the 'Xiduofeng ' that this method and Chinese patent 91104162 disclose is similar, different is, go up the present invention for 2 of 5-phenyl in 5-phenyl-pyrazolopyrimidine main body and adopted the product of fluorine replacement to be connected, and then the fluorine replacement is made 'Xiduofeng ' with oxyethyl group with the piperazine group.Preparation method of the present invention has improved yield, has simplified technology, has reduced cost, is adapted at China and produces the 'Xiduofeng ' product.
The present invention realizes by following route:
The invention will be further described for following examples: embodiment:
The preparation ice bath cooling of 1-methyl-4-nitro-3-n-propyl pyrazoles-5-formyl-2-fluorobenzoyl imines down, to be dissolved with the dichloromethane solution 100ml of 16.0g (0.1mol) 2-fluorobenzoyl chloride, be added drop-wise to during the methylene dichloride that 100ml contains 8.4g (0.04mol) 1-methyl-4-nitro-3-n-propyl pyrazoles-5-methane amide, 0.08g DMAP, 14.0ml (0.1ml) triethylamine/DMF mixes.Reinforced finishing, stirring reaction is 12 hours under the room temperature, and it is complete that TLC detects feedstock conversion, and it is poured in the 500ml distilled water, produces a large amount of solids, filter collection solid, washing.Filtrate is with dichloromethane extraction twice, merging filtrate, anhydrous magnesium sulfate drying filters, solvent evaporated under reduced pressure, faint yellow solid, heavy 8.6g, productive rate 65%, mp.89~90 ℃.Ultimate analysis (C
15H
15FN
4O
4) calculated value (%): C53.89, H4.49, N16.77, F5.69.Measured value (%): C54.02, H4.51, N16.77, F5.84.Mass spectrum (m/z): 335.1141 (molecular ion peaks).Proton nmr spectra: δ 1.02 (t, J=7.36,3H; n-propyl-CH3), δ 1.71~1.81 (m, 2H; first CH2 in the n-propyl), δ 2.93 (t, J=7.48; 2H, second CH2 in the n-propyl), δ 3.91 (s; 3H, NCH3), δ 7.21~7.24 (m; 1H, phenyl ring H), δ 7.30~7.35 (m; 1H, phenyl ring H), δ 7.62~7.65 (m; 1H, benzoyl contraposition H), δ 7.98~8.02 (m; 1H, benzoyl ortho position H), δ 9.73~9.76 (brs; 1H, CONHCO).Infrared absorption spectrum: 1730cm
-1(s ,-CONHCO-), 1694cm
-1(s ,-CONHCO-).5-(2-fluorophenyl)-1-methyl-3-n-propyl-1,6-dihydro-7H-pyrazolo [4,3-d] pyrimidine-7-ketone
Preparation the last imide derivative of 6.6g (0.02mol) is dissolved in the 10ml dehydrated alcohol, be warmed up to 65 ℃, stir then and add 27g (0.12mol) SnCl down in batches
2.2H
2O solid, feed rate hierarchy of control temperature did not surpass under 70 ℃ of temperature stirring reaction 2~3 hours, and it is complete that TLC detects feedstock conversion.With cool to room temperature, the frozen water cooling drips 2mol.L down
-1The NaOH aqueous solution is regulated pH7~8,4 * 100ml methylene dichloride, and anhydrous magnesium sulfate drying 12 hours filters, and removes solvent under reduced pressure, gets white powder, heavy 4.6g, and productive rate is 81%.mp161—163℃。Ultimate analysis: theoretical value (%): C62.94, H5.24, N19.58, F6.64.Measured value: C62.82, H5.26, N19.52, F6.70.Mass spectrum (m/z): 287.1298 (molecular ion peaks).Proton nmr spectra: δ 1.03 (t, J=7.36,3H; n-propyl-CH3), δ 1.81~1.91 (m, 2H; first CH2 in the n-propyl), δ 2.93 (t, J=7.48; 2H, second CH2 in the n-propyl), δ 4.27 (s; 3H, NCH3), δ 7.18~7.24 (m; 1H, phenyl ring H), δ 7.32~7.36 (m; 1H, phenyl ring H), δ 7.50~7.52 (m; 1H, benzoyl contraposition H), δ 8.28~8.33 (m; 1H, benzoyl ortho position H), δ 9.76~9.79 (s; 1H, CONH).Infrared absorption spectrum: 1693cm
-1(s ,-CONH-).5-[2-fluorine-5-(4-methylpiperazine base alkylsulfonyl) phenyl]-methyl]-1-methyl-3-n-propyl-1,6-
Dihydro-7H-pyrrole, joins 6.45g (0.024mol) previous step products therefrom in the 18ml chlorsulfonic acid also under the preparation room temperature of [4,3-d] pyrimidine-7-ketone than azoles in batches, and reinforced finishing is elevated to 50-60 ℃ with system temperature.Reacted 2 hours, cool to room temperature adds the 6.5ml sulfur oxychloride then, at room temperature stirred 4 hours, stopped reaction will react and mix thing slowly in the impouring 260g trash ice, use 250ml and 125ml dichloromethane extraction respectively, merge extraction, with the washing of 125ml saturated sodium-chloride water solution, behind the anhydrous sodium sulfate drying, filter, solvent evaporated under reduced pressure gets the canescence powder, add the 40ml methylene dichloride and make it dissolving, to wherein dripping 0.9g (8.89 * 10
-3Mol) triethylamine and 1.4g (0.014mol) N-methylpiperazine.Reinforced finishing continued stirring reaction 2 hours under the room temperature, and it is complete that TLC detects feedstock conversion, with the washing of 45ml saturated aqueous sodium carbonate, anhydrous magnesium sulfate drying, concentrate white solid 7.87g, productive rate 78%, mp172~173 ℃.Ultimate analysis: theoretical value (%): C53.57, H5.58, N18.75, F4.24, S7.14.Measured value: C53.29, H5.61, N18.60, F4.39, S7.20.Mass spectrum (m/z): 449.1754 (molecular ion peaks).Proton nmr spectra: δ 1.02 (t, J=7.36,3H, n-propyl-CH3); δ 1.81~1.91 (m, 2H, first CH2 in the n-propyl), δ 2.30 (t; J=7.48,2H, piperazine nitrogen methyl hydrogen), δ 2.53 (t; J=4.80,4H, n-formyl sarcolysine cardinal extremity CH2 on the piperazine ring), δ 2.93 (t; J=7.44,2H, second CH2 in the n-propyl), δ 3.15 (brs; 4H, sulphonyl cardinal extremity CH2 on the piperazine ring), δ 4.28 (s, 3H; nitrogen methyl hydrogen on the pyrazoles ring), δ 7.39 (dd, J1=8.64Hz, J2=11.56Hz; 1H, phenyl ring H), δ 7.88~7.92 (m; 1H, phenyl ring H), δ 8.68 (dd; J1=2.44Hz, J2=6.14Hz, phenyl ring H).Infrared absorption spectrum: 1702cm-1 (s ,-CONH-).5-[2-oxyethyl group-5-(4-methylpiperazine base alkylsulfonyl) phenyl]-methyl]-1-methyl-3-n-propyl-
1,6-dihydro-7H-pyrrole is than the also preparation of [4,3-d] pyrimidine-7-ketone of azoles
With 4.5g (0.01mol).The previous step reaction product is dissolved in 50ml N-methyl-2-pyrrolidone, adds 6.8g (0.1mol) sodium ethylate, and in 80 to 85 ℃ were reacted 6 hours, it is complete that TLC detects feedstock conversion, with the reaction mixture cool to room temperature, immerses in the 600ml water, with 4 * 100ml methylene dichloride united extraction liquid, the washing of 100ml saturated sodium-chloride water solution, anhydrous magnesium sulfate drying, filter, solvent evaporated under reduced pressure gets the white powder solid, heavy 3.18g, fusing point is 187 to 188 ℃, productive rate 67%.The structural analysis data see Appendix 2.
The preparation of Citric Acid 'Xiduofeng ' mixes previous step gained free alkali 50g with Citric Acid 20g, add 240ml water, the heating jolting adds the 240ml dehydrated alcohol then, and heating closely refluxes, activated carbon decolorizing, filtrate is cooled to room temperature and places, with the solid suction filtration of separating out, and the dry solid 58g that gets, mp.192~194 ℃, yield 82.8%.
Claims (4)
1. the method for preparing structural formula (1) compound:
Described method is represented with following reaction formula:
2. according to the method for claim 1, its end product methylene dichloride recrystallization.
Structure as shown in the formula compound:
Structure as shown in the formula compound:
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CNB991093453A CN1134441C (en) | 1999-06-28 | 1999-06-28 | Process for preparing sypolyphenol |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| CNB991093453A CN1134441C (en) | 1999-06-28 | 1999-06-28 | Process for preparing sypolyphenol |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| CN1279238A true CN1279238A (en) | 2001-01-10 |
| CN1134441C CN1134441C (en) | 2004-01-14 |
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| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CNB991093453A Expired - Fee Related CN1134441C (en) | 1999-06-28 | 1999-06-28 | Process for preparing sypolyphenol |
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| Country | Link |
|---|---|
| CN (1) | CN1134441C (en) |
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1999
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Address after: 100036 Beijing city Haidian District Cuiwei Road No. 4 Building No. 12, No. 4102 Yiyuanju Patentee after: Liu Yuan Address before: 100032 Ping On Mansion, No. 23, Xicheng District, Beijing, 718, Financial Street Patentee before: Sanxiong Hi-Tech Development Co Ltd, Beijing |
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