2-胺基-苯駢[e][1,3] -4-酮衍生物合成及中樞神經系統活性之研究
Synthesis of 2-Amino-Benzo[e][1,3]thiazin-4-ones Derivatives and Studies of Their Central Nervous System Activities
中文摘要
本論文乃在探討 2-胺基-苯駢[e][1,3] -4-酮化合物衍生物合成方法。以 2-甲硫基-苯駢 [e][1,3] -4-酮做為起始物,以不同胺基化合物進行取代反應,胺基化合物包括氨水、丁胺、
辛基胺、羥胺、3-氨基-1-丙醇、乙二胺、二甲縮醛胺、氮,氮-二甲基乙二胺、三乙胺、呱啶、
二乙二胺、氮-乙基-二乙二胺、1,4-氧氮六圜、2-甲醇- 咯烷、苯胺和對乙氧基苯胺等。反應 在室溫中進行,以甲醇為溶媒,經 6-48 小時之後,即可得到各式產物。所得產物經再結晶純化 後,由熔點測定、紅外線、質譜儀分析、核磁共振等光譜分析,判定其結構為 2-胺基-苯駢 [e][1,3] -4-酮類化合物,產率約在 60~90%。
將製備的 2-胺基-苯駢[e][1,3] -4-酮化合物 4、5、8、9、11 和 14 分別送測中樞神經藥 理活性評估,在麩胺酸受體及 γ-胺基丁酸受體藥理實驗中,發現對於麩胺酸受體結合能力,化 合物 9 及 14 分別為 20.09%和 19.06%的抑制作用比對照組 5,5-二氫內醯臆 甘醇醯
5.10%
為佳。對 γ-胺基丁酸-A 受體接受器[3H]muscimol 結合抑制作用中,化合物 9 抑制 作用為 28.41%比對照組苯妥因 4.35%為佳,然而化合物 5 和 8 卻呈現相反作用,抑制作用 分別為-10.89%和-15.84%。而正值數值越高,表示與受體結合能力越強,將來可以繼續研究 化合物屬於致效劑或拮抗劑;而負值的意義可能因受體蛋白質結構改變而造成的結果。
英文摘要
A facile synthesis of 2-amino-benzo[e][1,3]thiazin-4-one derivatives was achieved. A methanolic solution of 2-methylsulfanyl-benzo[e][1,3]
thizin-4-one was treated with various amine compounds at 25℃. The amine compounds are ammonia water, n-butylamine, n-octylamine, hydroxylamine, 3-aminopropanol, ethylenediamine, N,N-dimethylethyl- enediamine,
aminoacetaldehyde dimethylacetal, triethylamine, piperidine, piperazine, N-ethylpiperazine, morpholine, (S)-(+)-2-methanol- pyrrolidine, aniline, and p-phenetidine. The reaction completed in 6 to 48 hours, and the recrystallized products were identified with melting point measurement, IR, MS, 1H and 13C nuclear magnetic resonance spectroscopic analyses. The yields were between 60 to 90%.
Initially, six analogues including 4, 5, 8, 9, 11 and 14 were submitted for central nervous system activity assay by using glutamate receptor and
gamma-aminobutylamine receptor binding inhibition methods. The glutamate receptor binding inhibition method showed that compounds 9 and 14 demonstrated 20.09% and 19.06% were more active than that 5,5-dihydro-hydantoin
demonstrated 5.10%. On the other hand, in the gamma-aminobutylamine-A
receptor [3H]muscimol binding assay showed that compound 9 demonstrated 28.41% was more active than that dilantin demonstrated 4.35%. Compounds 5 and 8 were the other action to the gamma-aminobutylamine-A receptor [3H]muscimol binding assay that demonstrated —10.89% and —15.84%.