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易患显性遗传性癌症个体的正常皮肤成纤维细胞中肌动蛋白的生化特性改变。

Altered biochemical properties of actin in normal skin fibroblasts from individuals predisposed to dominantly inherited cancers.

作者信息

Antecol M H, Darveau A, Sonenberg N, Mukherjee B B

出版信息

Cancer Res. 1986 Apr;46(4 Pt 1):1867-73.

PMID:3948169
Abstract

The data presented here show that normal skin fibroblasts from individuals with dominantly inherited retinoblastoma, polyposis coli, and nevoid basal cell carcinoma (predisposed cells), grown in the presence of [35S]methionine, contain more than 2.5-fold [35S]methionine-labeled actin as compared to normal fibroblasts from individuals without a prior history of predisposition to cancer (normal cells). The rate of incorporation of [35S]methionine into actin in predisposed cells is rapid and is not correlated with an increase in the total protein and actin contents of the cells, in the intracellular pool size of [35S]methionine, or in the synthesis of beta-actin-specific mRNA, as compared to normal cells. However, the half-life of actin in predisposed cells is less than 5 h, as compared to at least 48 h for normal cells. The significantly reduced half-life of actin and an increased incorporation of [35S]methionine specifically into actin in all predisposed cells studied may represent an inherited biochemical defect which leads to cytoskeletal disorganization previously observed in these cells. It can be speculated that the altered properties of actin in predisposed cells may be caused by the same genetic lesion(s) which is responsible for the induction of dominantly inherited cancers.

摘要

此处呈现的数据表明,来自患有显性遗传性视网膜母细胞瘤、结肠息肉病和痣样基底细胞癌的个体(易感细胞)的正常皮肤成纤维细胞,在[35S]甲硫氨酸存在的情况下生长时,与没有癌症易感性病史的个体的正常成纤维细胞(正常细胞)相比,含有超过2.5倍的[35S]甲硫氨酸标记的肌动蛋白。与正常细胞相比,易感细胞中[35S]甲硫氨酸掺入肌动蛋白的速率很快,且与细胞总蛋白和肌动蛋白含量的增加、[35S]甲硫氨酸的细胞内池大小或β-肌动蛋白特异性mRNA的合成无关。然而,易感细胞中肌动蛋白的半衰期小于5小时,而正常细胞至少为48小时。在所有研究的易感细胞中,肌动蛋白半衰期的显著缩短以及[35S]甲硫氨酸特异性掺入肌动蛋白的增加,可能代表一种遗传性生化缺陷,这种缺陷导致了先前在这些细胞中观察到的细胞骨架紊乱。可以推测,易感细胞中肌动蛋白特性的改变可能是由导致显性遗传性癌症发生的相同遗传损伤引起的。

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