T Shimizu, Y Ohtsuka, Y Yanagihara, M Kurimura, M Takemoto, K Achiwa
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引用次数: 0
摘要
四种化学合成的脂肽类似物S-[2,3-二(棕榈酰氧基)- 2r(称为KAB-1), - 2s (KAB-3)-丙基]- n -[2,3-二(棕榈酰氧基)- 2r (S)-丝氨酸-(S)-丝氨酸-(S)-丝氨酸-(S)-天冬酰胺-(S)-丙氨酸]- n -[(2,2,2)-三氯乙氧基]-(R)-半胱氨酸-(S)-丝氨酸-(S)-丝氨酸-(S)-丝氨酸-(S)-丝氨酸]和- 2s (KAB-4)-丙基]-(R)-半胱氨酸-(S)-丝氨酸-(S)-丝氨酸-(S)-丝氨酸-(S)-天冬酰胺-(S)-丙氨酸,对细菌脂蛋白进行了研究。这四种类似物以及细菌脂多糖(LPS)或合成大肠杆菌型脂质A(506)均能使[3H]胸腺嘧啶进入C3H/He小鼠脾细胞。虽然LPS和506在C3H/HeJ小鼠中没有表现出有丝分裂活性,但KAB化合物表现出显著的有丝分裂性。这些类似物对半乳糖胺负荷的C57BL/6小鼠在50微克/只的高剂量下没有显示出致死毒性。四种类似物刺激腹腔巨噬细胞产生TNF,诱导L929细胞体外裂解。两次静脉注射50微克/只这些类似物,对BALB/c小鼠甲胺磷A纤维肉瘤的生长有微弱的抑制作用。在4种类似物中,KAB-2化合物的抑制作用最强,具有较强的tnf诱导作用。这些结果表明,KAB-2(甘油部分C-2位与双棕榈酰的r构型)的生物活性比其他三种类似物强。
Comparison of biologic activities of synthetic lipopentapeptide analogs of bacterial lipoprotein in mice.
Mitogenicity, lethal toxicity, induction of tumor necrotizing factor (TNF), and antitumor activity against Meth A fibrosarcoma of four chemically synthesized lipopentapeptide analogs, S-[2,3-bis(palmitoyloxy)-2R (designated as KAB-1), -2S(KAB-3)-propyl]-N-palmitoyl-(R)-cysteinyl-(S)-seryl- (S)-seryl-(S)-asparaginyl-(S)-alanine, S-[2,3-bis(palmitoyloxy)-2R(KAB-2), and -2S(KAB-4)-propyl]-N-[(2,2,2)-trichloroethoxycarbonyl]-(R)- cysteinyl-(S)-seryl-(S)-seryl-(S)-asparaginyl-(S)-alanine, of bacterial lipoprotein were investigated. These four analogs, as well as bacterial lipopolysaccharide (LPS) or synthetic Escherichia coli-type lipid A (506), were capable of increasing of [3H]thymidine into splenocytes of C3H/He mice. Although LPS and 506 did not exhibit the mitogenic activity in C3H/HeJ mice, KAB compounds showed remarkable mitogenicity. These analogs did not show the lethal toxicity at a high dose of 50 micrograms/mouse in galactosamine-loaded C57BL/6 mice. Peritoneal macrophages, stimulated with four analogs, caused the production of TNF which induces the L929 cell lysis in vitro. Twice, intravenous injections of 50 micrograms/mouse of these analogs showed weak growth inhibition of Meth A fibrosarcoma in BALB/c mice. The inhibitory effect of KAB-2 compound, which caused the strong TNF-induction among the four analogs, was the most potent. These results indicate that the biological activity of KAB-2 (R-configuration of the C-2 position in glycerol moiety with dipalmitoyl) is stronger than that of the other three analogs.