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决定分裂:细胞是如何做出决定的?

Determining to divide: how do cells decide?

作者信息

Smith Kendall A

机构信息

The Division of Immunology, Department of Medicine, Weill Medical College, Cornell University, New York, NY U.S.A.

出版信息

J Biol Phys. 2005 Dec;31(3-4):261-72. doi: 10.1007/s10867-005-6060-x.

Abstract

A cell's decision to divide must be regulated with the highest fidelity. Otherwise, abnormalities occurring in the replication of genetic material and cytokinesis would be incompatible with life. It has been known for almost a century that cells comprising a population undergo cellular division at extremely variable rates, even though genetically identical cell clones have been examined. Studies with T lymphocytes at the single cell level have revealed that the rate of cellular division is determined by the accumulation of a critical number of ligand-triggered interleukin-2 (IL2) receptors at the cell surface throughout the G(1) phase of the cell cycle. Thus, the cell "counts" the number of triggered IL2 receptors, and only decides to divide when the critical number has been attained. This information is then transferred to the cellular interior via intracellular sensors comprised of D-type cyclins, which ultimately determine when the cell surpasses the "Restriction Point" in late G(1), and which commits the cell irrevocably to initiate DNA replication. Beyond the R-point, the cell assembles a definite number of macromolecular pre-replication complexes (Pre-RCs) comprised of at least 6 distinct proteins at sites of the origin of replication on DNA. Complete assembly of the Pre-RCs is a prerequisite for their subsequent disassembly, which must occur before the initiation of DNA strand replication, and which occurs asynchronously throughout the S-phase of the cell cycle and only terminates when the entire DNA has been duplicated. Thus, the fidelity of the decision to divide is exquisitely regulated by macromolecular mechanisms initiated at the cell surface and transferred to the cellular interior so that the cell can make the decision in a quantal (all-or-none) fashion. The question before us is how this quantal decision is made at the molecular level. The available data indicate that the assembly and disassembly of a definite number of large multicomponent macromolecular complexes make the quantal decisions. Here, it is postulated that all fundamental cellular decisions, i.e. survival, death, proliferation and differentiation, are regulated in this fashion. It remains to be determined how the cell counts the signals it receives, and what the molecular forces are that dictate the behavior of macromolecular complexes.

摘要

细胞分裂的决定必须以最高的保真度进行调控。否则,遗传物质复制和胞质分裂过程中出现的异常将与生命不相容。近一个世纪以来,人们已经知道,即使研究的是基因相同的细胞克隆,组成群体的细胞进行细胞分裂的速率也极为不同。对单细胞水平的T淋巴细胞的研究表明,细胞分裂速率是由在细胞周期的G1期整个过程中细胞表面积累的关键数量的配体触发的白细胞介素-2(IL2)受体所决定的。因此,细胞“计数”被触发的IL2受体的数量,只有在达到关键数量时才决定分裂。然后,这些信息通过由D型细胞周期蛋白组成的细胞内传感器传递到细胞内部,这些传感器最终决定细胞在G1晚期何时超过“限制点”,并使细胞不可逆转地开始DNA复制。超过限制点后,细胞在DNA复制起点处组装一定数量的由至少6种不同蛋白质组成的大分子前复制复合物(Pre-RCs)。Pre-RCs的完整组装是其随后拆卸的先决条件,拆卸必须在DNA链复制开始之前发生,并且在细胞周期的S期异步发生,只有当整个DNA被复制时才终止。因此,分裂决定的保真度由始于细胞表面并传递到细胞内部的大分子机制精确调控,以便细胞能够以量子(全或无)方式做出决定。我们面临的问题是,这种量子决定在分子水平上是如何做出的。现有数据表明,一定数量的大型多组分大分子复合物的组装和拆卸做出了量子决定。在此假设,所有基本的细胞决定,即存活、死亡、增殖和分化,都是以这种方式调控的。细胞如何计数其接收到的信号,以及决定大分子复合物行为的分子力是什么,仍有待确定。

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Determining to divide: how do cells decide?决定分裂:细胞是如何做出决定的?
J Biol Phys. 2005 Dec;31(3-4):261-72. doi: 10.1007/s10867-005-6060-x.

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