生死未卜

A J Dibenedetto, R N Pittman
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引用次数: 0

摘要

关于程序性细胞死亡的两个主要假设是,它是基因表达途径的最终结果,它是细胞对相互冲突的生长控制信号的反应。这些观点进行了检验,并讨论了它们在发育过程中神经元细胞死亡的潜在应用。由于大多数与细胞死亡有关的哺乳动物基因具有其他功能,因此有可能在哺乳动物中不存在一组新的死亡基因。相反,鉴定出的基因可能将最初的死亡刺激与实际导致死亡的细胞事件联系起来,主要是通过提供指导决定的调节信号。细胞死亡是对相互冲突的生长调节信号的反应,这一观点最初来源于对循环的非神经元细胞的研究,现在被应用于增殖的神经元前体和有丝分裂后神经元。神经元在发育过程中的死亡可能是相互冲突的信号的结果,以及视网膜母细胞瘤蛋白如何在不同的神经元群体中协商“冲突死亡”。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Death in the balance.

Two major hypotheses concerning programmed cell death are that it is the end result of a gene expression pathway and that it is the cellular response to conflicting growth control signals. These ideas are examined, and their potential applicant to neuronal cell death during development is discussed. Since most mammalian genes involved in cell death have other functions, it is possible that a novel set of death genes does not exist in mammals. Instead, the genes identified may serve to link an initial stimulus to die with the cellular events that actually cause death, primarily by providing regulatory signals that direct the decision. The idea of cell death as a response to conflicting growth regulatory signals, initially derived from studies on cycling, non-neuronal cells, is applied to proliferating neuronal precursors and postmitotic neurons. How neuronal death during development might be the outcome of conflicting signals, and how retinoblastoma protein might negotiate "death by conflict" in different populations of neurons is discussed.

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