首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Studies on mechanism of action of anti-tumor-promoting agents: their specificity in two-stage promotion.
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Studies on mechanism of action of anti-tumor-promoting agents: their specificity in two-stage promotion.

机译:抗肿瘤促进剂作用机理的研究:它们在两阶段促进中的特异性。

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摘要

The effects of fluocinolone acetonide (FA), retinoic acid (RA), and tosylphenylalanine chloromethyl ketone (TPCK) on two-stage promotion after 7,12-dimethylbenz[a]-anthracene (DMBA) initiation in female Sencar mice were investigated. The two-stage promotion protocol was achieved by twice weekly applications of 2 microgram of 12-O-tetradecanoylphorbol 13-acetate (TPA) for 2 weeks (stage I) followed by twice weekly applications of mezerein for 18 weeks (stage II). Separately stage I and II do not cause any tumors to develop after DMBA initiation. FA was found to be a potent inhibitor of stages I and II but to a greater degree for stage I than for stage II. RA was ineffective in stage I but was a potent inhibitor of stage II; TPCK specifically inhibited stage I but not stage II. FA and TPCK effectively counteract the appearance of the dark basal keratinocytes, whereas RA has no effect. These results provide additional evidence for the importance of dark basal keratinocytes in stage I of promotion and indicate that most of the other biochemical and morphological responses normally associated with promotion (such as polyamines) are actually associated with stage II of promotion.
机译:研究了氟喹诺酮(FA),视黄酸(RA)和甲苯磺酰基苯丙氨酸氯甲基酮(TPCK)对雌性Sencar小鼠7,12-二甲基苯并[a]-蒽(DMBA)启动后的两阶段促进作用。通过每周两次应用2微克12-O-十四烷酰佛波醇13-乙酸盐(TPA)两次,持续2周(阶段I),然后每周两次应用美泽林,持续18周(阶段II),实现了两阶段促进方案。在DMBA启动后,单独的I和II期不会引起任何肿瘤的发展。发现FA是I和II期的有效抑制剂,但是I期比II期在更大程度上是FA。 RA在I期无效,但是II期的有效抑制剂。 TPCK特异性抑制I期,但不抑制II期。 FA和TPCK可有效抵消深色基底角质形成细胞的出现,而RA无作用。这些结果提供了额外的证据,表明在促进的第一阶段,深色基底角质形成细胞的重要性,并表明通常与促进有关的大多数其他生化和形态反应(如多胺)实际上与促进的第二阶段有关。

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