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增殖寿命检查点:细胞类型特异性及其对肿瘤生物学的影响

Proliferative lifespan checkpoints: cell-type specificity and influence on tumour biology.

作者信息

Wynford-Thomas D

机构信息

Department of Pathology, University of Wales College of Medicine, Cardiff, U.K.

出版信息

Eur J Cancer. 1997 Apr;33(5):716-26. doi: 10.1016/S0959-8049(97)00064-6.

Abstract

Lifespan checkpoints are viewed here as intrinsic mechanisms which desensitise cells to external growth signals as a programmed response to proliferative age, as distinct from externally-triggered differentiation. This review focuses on the role of tumour suppressor gene products as essential mediators of cell cycle arrest at lifespan checkpoints, concentrating in particular on p53. Although drawing inevitably on fibroblast senescence and telomere erosion paradigms, other lifespan clocks and signal pathways are discussed. Particular emphasis is placed on cell-type diversity in the nature, number and timing of lifespan checkpoints and its importance for tumour biology. Breast and thyroid cancer are used to illustrate the concept that the "choice" of checkpoint(s) in a given normal cell may have a determining influence on the mutational spectrum and clinical behaviour of its tumours.

摘要

寿命检查点在这里被视为一种内在机制,它使细胞对外部生长信号不敏感,作为对增殖年龄的一种程序性反应,这与外部触发的分化不同。本综述重点关注肿瘤抑制基因产物作为寿命检查点处细胞周期停滞的重要介质的作用,尤其集中在p53上。虽然不可避免地借鉴了成纤维细胞衰老和端粒侵蚀范式,但也讨论了其他寿命时钟和信号通路。特别强调了寿命检查点在性质、数量和时间上的细胞类型多样性及其对肿瘤生物学的重要性。乳腺癌和甲状腺癌被用来说明这样一个概念,即在给定的正常细胞中“选择”检查点可能对其肿瘤的突变谱和临床行为产生决定性影响。

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