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Tumor promoter induces sister chromatid exchanges: relevance to mechanisms of carcinogenesis.

机译:肿瘤启动子诱导姐妹染色单体交换:与致癌机制有关。

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摘要

12-O-Tetradecanoylphorbol 13-acetate (TPA), a powerful tumor promoter, is shown to induce sister chromatid exchanges (SCEs), whereas the nonpromoting derivative 4-O-methyl-TPA does not. Inhibitors of tumor promotion--antipain, leupeptin, and fluocinolone acetonide--inhibit formation of such TPA-induced SCEs. TPA is a unique agent in its induction of SCEs in the absence of DNA damage, chromosome aberrations, mutagenesis, or significant toxicity. Because TPA is known to induce several gene functions, we speculate that it might also induce enzymes involved in genetic recombination. Thus, the irreversible step in tumor promotion might be the result of an aberrant mitotic segregation event leading to the expression of carcinogen/mutagen-induced recessive genetic or epigenetic chromosomal changes.
机译:12-O-四氢碳酰佛波醇13-乙酸盐(TPA)是一种强大的肿瘤启动子,可诱导姐妹染色单体交换(SCE),而非促进性衍生物4-O-甲基-TPA则不能。促进肿瘤的抑制剂-抗痛药,亮肽素和氟轻松-丙酮酸-抑制此类TPA诱导的SCE的形成。在没有DNA损伤,染色体畸变,诱变或明显毒性的情况下,TPA是诱导SCE的独特药物。因为已知TPA会诱导几种基因功能,所以我们推测它也可能会诱导参与基因重组的酶。因此,肿瘤促进中不可逆的步骤可能是异常有丝分裂分离事件的结果,该事件导致表达致癌物/诱变剂引起的隐性遗传或表观遗传染色体改变。

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