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端粒功能障碍导致的染色体重排及其在癌症中的作用。

Chromosome rearrangements resulting from telomere dysfunction and their role in cancer.

作者信息

Murnane John P, Sabatier Laure

机构信息

Radiation Oncology Research Laboratory, University of California, San Francisco, CA 94103, USA.

出版信息

Bioessays. 2004 Nov;26(11):1164-74. doi: 10.1002/bies.20125.

Abstract

Telomeres play a vital role in protecting the ends of chromosomes and preventing chromosome fusion. The failure of cancer cells to properly maintain telomeres can be an important source of the chromosome instability involved in cancer cell progression. Telomere loss results in sister chromatid fusion and prolonged breakage/fusion/bridge (B/F/B) cycles, leading to extensive DNA amplification and large deletions. These B/F/B cycles end primarily when the unstable chromosome acquires a new telomere by translocation of the ends of other chromosomes. Many of these translocations are nonreciprocal, resulting in the loss of the telomere from the donor chromosome, providing a mechanism for transfer of instability from one chromosome to another until a chromosome acquires a telomere by a mechanism other than nonreciprocal translocation. B/F/B cycles can also result in other forms of chromosome rearrangements, including double-minute chromosomes and large duplications. Thus, the loss of a single telomere can result in instability in multiple chromosomes, and generate many of the types of rearrangements commonly associated with human cancer.

摘要

端粒在保护染色体末端和防止染色体融合方面发挥着至关重要的作用。癌细胞无法正确维持端粒可能是癌细胞进展过程中染色体不稳定的一个重要来源。端粒缺失会导致姐妹染色单体融合以及延长的断裂/融合/桥接(B/F/B)循环,从而导致广泛的DNA扩增和大片段缺失。这些B/F/B循环主要在不稳定的染色体通过其他染色体末端的易位获得新的端粒时结束。许多这些易位是非相互性的,导致供体染色体上的端粒丢失,提供了一种将不稳定性从一条染色体转移到另一条染色体的机制,直到一条染色体通过非相互性易位以外的机制获得端粒。B/F/B循环还可导致其他形式的染色体重排,包括双微体染色体和大片段重复。因此,单个端粒的缺失可导致多条染色体的不稳定,并产生许多通常与人类癌症相关的重排类型。

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