• 专利附录
  • 专利说明
  • 权利要求
  • 类似技术
  • 同族专利
  • 引用文献
  • 法律状态
  • 优先权
    • 专利摘要:
    Cinnamamide compounds of the formula <IMAGE> where X is chloro, bromo or iodo and R is hydrogen or alkyl of 1 to 3 carbons AS PHARMACEUTICALS WHICH ARE USEFUL IN THE TREATMENT OR PROPHYLAXIS FOR CONVULSIONS.
    公开号:SU728712A3
    申请号:SU752163175
    申请日:1975-08-08
    公开日:1980-04-15
    发明作者:Майкл Гривски Юджин
    申请人:Дзе Велкам Фаундейшн Лимитед (Фирма);
    IPC主号:
    专利说明:

    one
    This invention relates to organic chemistry, specifically to a process for the preparation of cinnamic acid agna of general formula I
    X sensok ,,
    where X is chlorine, bromine or iodine, R is hydrogen or C-Cd-alkyl, provided that if X is chlorine, then R is not hydrogen.
    These compounds in animal experiments have anticonvulsant activity, which suggests the possibility of their use in medicine.
    A known method for producing amides of various acids by acylation of amines with acids or their reactive derivatives at elevated temperatures, however, no compound I / I was obtained, where R and X would have given values having physiological activity 1.
    The aim of the invention is a process for the preparation of new cinnamic acid amide compounds of the general formula I, where X and R have the meanings having physiological activity.
    The goal is achieved by the described method for the preparation of cinnamic acid amide of the general formula I, where X and R have the given meanings, consisting in that the compound form "Uhl, E
    where R - is as defined, W is hydrogen, CONHg, CO -, is acylated with an acid of the formula and
     CH CH - COOK
    where X has the stated values, or its reactive derivative at a temperature, from room temperature to boiling of the reaction mass. Preferably, as the reactive derivative of the acid w, its chlorine anhydride or the alkyl ester is taken; preferably, the process is conducted in an inert organic solvent — benzene, toluene, sulfuric ether, or mixtures thereof.
    The process technology is that a compound of the formula TJ is mixed with an acid of the formula (I, its acid chloride or Cd-alkyl ester. If necessary, an inert solvent, benzene, toluene is used.
    sulfuric ether, methanol or their mixture, and the process is carried out at room temperature or at boiling of the reaction mass.
    Example 1. 3-Bromo-N-isopropyl cinnamamide. To a solution of 11.4 g of trans-bromocinnamic acid in boiling dry benzene (75 ml) was added a mixture of thionyl chloride (12 g) and dry benzene at such a rate as to maintain boiling; the mixture is then refluxed for another 2 hours. The solvent and excess thionyl chloride are distilled off under reduced pressure to obtain Trans-3-bromo-cinnamoyl chloride (12.3 g). A solution of 3-bromo-cinnamoyl chloride in toluene (150 ml) is added dropwise with stirring to a solution of isopropylamine (10 g) in ether (200 ml), the reaction mixture is stirred at room temperature for 1 hour and then heated for 1 hour under reflux. . The solvent and the excess amine are removed under reduced pressure. The crude residue is treated with water, the precipitate is filtered and recrystallized from a mixture of water and ethanol to give crystalline 3-bromo-L-isopropyl cinnamine with a m.p. 85-8b C. Elemental analysis and UV and NMR spectra confirm the structure of the product.
    Example 2, 3-Bromo-N-ethylcinnamamide.
    A solution of trans-3-bromocinnamoyl chloride (12.3 g) in anhydrous toluene (150 ml) was slowly added with stirring to a solution of ethylamine (10 g) in dry ether at room temperature. The reaction mixture is heated under reflux for 1 hour and then the solvent and the excess amine are removed under reduced pressure. The residue is treated with water, filtered, recrystallized from ethanol-water and to obtain trans-Z-bromo-N-ethylcinnamamide with so pl. .89-90 ° C. The UV and NMR spectra, as well as elemental analysis, confirm its structure.
    Example 3. 3-Bromo-Y-ethylcinnamamide.
    The trans-meta-bromcinnucus acid) (14.8 g), ethanol (173 ml) and concentrated sulfuric acid (0.4 ml) are mixed and the mixture is heated under reflux for 15 hours. About 150 ml of ethanol are distilled off and the residue is poured into ice and water (140 ml). The cold mixture is alkalinized with 40% sodium hydroxide and extracted with methylene chloride {4 60 mp). The combined extracts are dried over anhydrous potassium carbonate. Carbonic acid potassium: filtered and the solvent evaporated under reduced pressure. -Trans-ethyl-3-brominenamate is also obtained in the form of partially solidified oil
    (IR spectrum corresponds to this compound).
    The trans ethyl 3-bromocinnamate (8.4 g), ztilamine (6.7 g), methanol (18 ml) and 4D molecular sieve (1 g) are mixed and heated under reflux for half an hour. The mixture is cooled to 45 ° C and methyl catree (0.6 g) is added, the mixture is then heated for 1.5 hours, cooled and acidified with concentrated hydrochloric acid (12 m-p), and the molecular sieve is filtered. Ice-cold water was added to the filtrate. The precipitation of trans-3-bromo-L-ethylcinnamamide B, which, after crystallisation from ethanol, has a mp. 89-90 ° C.
    Example 4. 3-Bromo-Y-methyl (Zinnaglamide.
    A solution of Tpof 14 with - 3-bromocin, nam l chloride (5 g) In dry benzene (100 ml) is added to ether (200 tvui) solution of methylamine (3 g). At the end of the addition, a weak current of methylamine gas is passed through the reaction mixture at room temperature for 1 hour. The solvent and the excess amine are removed under reduced pressure. The crude product is treated with water, filtered, recrystallized from ethanol-water, and trans-Z-bromo-N-methylcinnamamide is obtained, with t, tnp. 147-147, 3 The UV and NMR spectra and elemental analysis confirm its structure.
    Example 5. 4-Chloro-ethylcinnamamide.
    According to the method; Example 2 is subjected to the reaction of the throne-3-chloro-cinnamoyl chloride (4.4 g) in dry benzene (75 ml) with an excess of ethylamine in dry ether (75 ml) and trans-3-chloro-N-ethylcinnamamide with m.p. 87-88 ° C. The structure is confirmed by elemental analysis and UV and NMR spectra.
    Example 6. Z-Iod-N-ethylcinnamamide.
    (MeTa-iodo-cinnamoyl chloride is obtained from G | S101-ethyl-iodicoric acid by the standard procedure of Example 1. This acid chloride (6.6 g) in dry toluene (200 ml) is added with stirring to a solution of ethylamine (3.0 g) in dry ether (300 ml} at room temperature. The reaction mixture is heated under reflux for 1 hour and then treated according to Example 2, and grons-ylets-iodine-N-ethylcinnamamide with mp 116-117 ° C is obtained in the form of a white crystalline material.
    Elemental analysis and the UV and NMR spectra confirm its structure.
    Examples 7-10. Following the procedure of example 2, trout-compounds of general formula i are obtained (in all cases, the structure is confirmed by elemental analysis and by UV and NMR spectra), given in Table. one.
    Table 1. EXAMPLE 12-13. Following the procedure of examples 1 and 4, from 3-iodo-cinnamoyl chloride, throne compounds of the formula T are given in Table 2 121 CH (CH) 2109-110 131H134-135 in each case, the UV and NMR spectra and elemental analysis confirm the structure. Melting points are indicated.
    after recrystallization from ethanol-water.
     the invention
    1. The method of producing cinnamon amide to slots of the formula G
    X is t-CH HNSOCK where X is chlorine, bromine or iodine, R is hydrogen or C is Cd-alkyl, provided that if X is chlorine, then R is not hydrogen, they are also distinguished by the fact that a compound of the formula I R -NH- y where R has the indicated meanings; W is hydrogen, CONH2, CO is alkyl; They are acylated with an acid of formula from 1ГГ) СН СН-dooH where X - has the indicated values, or its reactive derivative at a temperature from room temperature to boiling of the reaction mass. 2. Method POP1, characterized in that its acid chloride or C-C-alkyl ester is taken as a reactive derivative of acid III. 3. Method according to paragraphs. 1, 2, about 1 t and that the acylation is carried out in an inert organic solvent — benzene, toluene, sulfuric ether, methanol, or mixtures thereof. Sources of information, rintye taken into account in the examination 1. K. Bksher, D. Pearson, Organic syntheses, Part 2, M. Mir, 1973, p.384.
    权利要求:
    Claims (3)
    [1]
    Claim
    1. The method of producing cinnamic acid amide of the formula I
    X cn = (Jhconhr where X is chlorine, bromine or iodine, R is hydrogen or Cf-C 3 -alkyl, provided that if X is chlorine, then R is not hydrogen, characterized in that the compound of formula
    R-Nh-mm where R has the indicated meanings, W EXAMPLE 12-13. Following the methods of examples 1 and 4, from 3-iodocinnamoyl chloride receive trone compounds of the formula T, are given in table. 2./ O hydrogen, CONH 2 , CO - alkyl; acylated with an acid of the formula [C
    SI = Sn-Soon where X - has the indicated meanings, or its reactive derivative at a temperature of room temperature
    table 2
    Example X R Mp. ° C 25 12 1 sn (sn 3 ) 2109-110 thirteen 1 n 134-135 thirty
    to the boil of the reaction mass.
    [2]
    2. The method of pop. 1, characterized in that as the reactive derivative of acid H take its acid chloride or
    C ^ -C-alkyl ether.
    [3]
    3. The method of I according to claims 1, 2, characterized in that the acylation is carried out in an inert organic solvent - benzene, toluene, sulfuric ether, methanol or their mixture. In each case, UV and NMR spectra and elemental analysis confirm the structure. Melting points are indicated by sakh.
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    同族专利:
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    引用文献:
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    GB1131727A|1966-05-10|1968-10-23|Smith Kline French Lab|Antidepressant n,n-dimethylcinnamamide compositions|
    GB1128142A|1966-06-30|1968-09-25|James Lincoln Bezemek|Wear indicating arrangement for vehicle power transfer devices|
    US3444197A|1966-09-27|1969-05-13|Upjohn Co|3,4-dihalocinnamamides|
    US3538156A|1967-07-24|1970-11-03|Herbert Schwartz|Cinnamamides|
    CH510019A|1968-11-05|1971-07-15|Thomae Gmbh Dr K|Antiphlogistic, antipyretic halo-cinnama-mides|
    CH532047A|1967-12-01|1972-12-31|Thomae Gmbh Dr K|Process for the preparation of new cinnamic acid amides|
    US3488749A|1968-01-29|1970-01-06|Smithkline Corp|Antidepressant n,n-dimethylcinnamamide compositions and methods|
    FR2040181A1|1969-04-02|1971-01-22|Lipha|
    CA1174865A|1971-04-16|1984-09-25|Ferenc M. Pallos|Thiolcarbamate herbicides containing nitrogencontaining antidote|US4190674A|1976-02-03|1980-02-26|Burroughs Wellcome Co.|3-Fluoro-N-cyclopropylcinnamide|
    US4107320A|1976-08-06|1978-08-15|Burroughs Wellcome Co.|Biologically active amides|
    US4183858A|1977-07-01|1980-01-15|Merrell Toraude Et Compagnie|α-Vinyl tryptophanes|
    US4179524A|1978-06-16|1979-12-18|Burroughs Wellcome Co.|Biologically active amide|
    DE4421536A1|1994-06-20|1995-12-21|Hoechst Ag|Phenyl-substituted alkenylcarboxylic acid guanidines bearing perfluoroalkyl groups, processes for their preparation, their use as medicaments or diagnostic agents, and medicaments containing them|
    KR100492809B1|2001-11-23|2005-06-03|한국화학연구원|4-hydroxycinnamamide derivatives as antioxidants, process for preparing thereof and pharmaceutical compositions containing them|
    PL209602B1|2005-10-20|2011-09-30|Inst Chemii Bioorg Pan|Synthesis of amide of the 3- propane acid|
    法律状态:
    优先权:
    申请号 | 申请日 | 专利标题
    GB35279/74A|GB1519762A|1974-08-09|1974-08-09|Cinnamamides their preparation and pharmaceutical compositions containing them|
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