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关于复制子“错误启动”的代谢控制可能性:与哺乳动物细胞谱系中恶性表型出现的关系。

On the possibility of metabolic control of replicon "misfiring": relationship to emergence of malignant phenotypes in mammalian cell lineages.

作者信息

Varshavsky A

出版信息

Proc Natl Acad Sci U S A. 1981 Jun;78(6):3673-7. doi: 10.1073/pnas.78.6.3673.

Abstract

Constraints of a multireplicon chromosomal organization and of the necessity to maintain constant gene dosages demand that each origin of replication in a eukaryotic cell "fire" (initiate replication) only once per cell cycle. The central idea of this work is that a low probability of an extra ("illegitimate") round of DNA replication (called below "replicon misfiring") within any given chromosomal domain could be increased by certain substances of either intra- or extracellular origin. The term " "firone" is proposed for such a substance. It is shown that existence of firones could greatly speed up evolution of cellular systems under selection pressure, a developing tumor being one example of such a system. Experimentally testable predictions of the firone hypothesis are discussed.

摘要

多复制子染色体组织的限制以及维持恒定基因剂量的必要性要求真核细胞中的每个复制起点在每个细胞周期仅“激发”(启动复制)一次。这项工作的核心观点是,细胞内或细胞外来源的某些物质可能会增加任何给定染色体区域内额外一轮(“非法”)DNA复制(以下称为“复制子误激发”)的低概率。为此类物质提出了“firone”一词。结果表明,firone的存在可以在选择压力下极大地加速细胞系统的进化,正在发展的肿瘤就是这样一个系统的例子。文中讨论了firone假说的可实验验证的预测。

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