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癌基因激活在小鼠皮肤肿瘤产前(经胎盘)起始和产后促进过程中的作用。

Role of oncogene activation during prenatal (transplacental) initiation and postnatal promotion of mouse skin tumours.

作者信息

Yamasaki H, Hollstein M, Cabral J R, Tomatis L

机构信息

International Agency for Research on Cancer Lyon, France.

出版信息

IARC Sci Publ. 1989(96):221-37.

PMID:2680947
Abstract

The transplacental initiation-postnatal promotion model of mouse skin carcinogenesis is useful in studying the molecular and cellular mechanisms of perinatal carcinogenesis. Offspring transplacentally exposed to an initiating dose of a carcinogen typically do not produce any skin tumours in the absence of postnatal treatment; many skin tumours appear only when they are treated with tumour-promoting agents postnatally. Tumour-promoting agents alone produce no skin tumours or only a few. Thus, two stages of carcinogenesis, initiation and promotion, can be conveniently separated. Our results indicate that fetal c-Ha-ras can be transplacentally activated through a specific point mutation by a carcinogen. However, since postnatal promotion was essential for the production of tumours, they also suggest that a cell harbouring such a mutation may remain dormant until it encounters a tumour-promoting stimulus. Since a higher fraction of carcinomas than papillomas contained the specific mutation in Ha-ras, it is postulated that those papillomas with the point mutation have a selective advantage to progress towards carcinomas.

摘要

小鼠皮肤癌发生的经胎盘启动-产后促进模型,对于研究围产期癌发生的分子和细胞机制很有用。经胎盘暴露于致癌剂启动剂量的子代,在没有产后处理的情况下通常不会产生任何皮肤肿瘤;只有在产后用肿瘤促进剂处理时,才会出现许多皮肤肿瘤。单独使用肿瘤促进剂不会产生皮肤肿瘤或只会产生少数肿瘤。因此,癌发生的两个阶段,即启动和促进,可以方便地分开。我们的结果表明,胎儿的c-Ha-ras可被致癌剂通过特定的点突变经胎盘激活。然而,由于产后促进对于肿瘤的产生至关重要,这些结果还表明,携带这种突变的细胞可能会一直处于休眠状态,直到遇到肿瘤促进刺激。由于癌组织中含有Ha-ras特定突变的比例高于乳头状瘤,因此推测那些具有点突变的乳头状瘤在向癌发展方面具有选择性优势。

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