Structure-activity studies on synthetic analogues (indolactams) of the tumor promoter teleocidin.

Gan Pub Date : 1984-10-01
H Fujiki, M Suganuma, M Nakayasu, T Tahira, Y Endo, K Shudo, T Sugimura
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引用次数: 0

Abstract

Synthetic analogues (indolactams) related to the tumor promoter teleocidin were synthesized chemically. Of four indolactam-Vs lacking the monoterpenoid moiety of native teleocidin, (-)-indolactam-V bound to the 12-O-tetradecanoylphorbol-13-acetate receptor in cell membranes and induced both adhesion of HL-60 cells and ornithine decarboxylase activity in mouse skin, although its effects were weaker than those of teleocidin. (+)-Indolactam-V and two isomers of epi-indolactam-V showed no induction of ornithine decarboxylase. These results indicate that the S,S configuration of native teleocidin at the isopropyl residue and the hydroxymethyl group is necessary for activity.

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肿瘤启动子远杀素合成类似物(吲哚内酰胺)的构效研究。
用化学方法合成了与肿瘤启动子远杀素相关的吲哚内酰胺类化合物。在四种缺乏天然远杀菌素单萜类部分的吲哚内酰胺- v中,(-)-吲哚内酰胺- v与细胞膜上的12- o -十四烷醇-13-乙酸受体结合,诱导HL-60细胞的粘附和小鼠皮肤上鸟氨酸脱羧酶的活性,尽管其作用弱于远杀菌素。(+)-吲哚内酰胺- v和两种外皮-吲哚内酰胺- v异构体对鸟氨酸脱羧酶无诱导作用。这些结果表明,在异丙基残基和羟甲基上的S,S构型对活性是必需的。
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