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正常细胞与异常细胞增殖。统一且分析性的概述。

Normal versus abnormal cell proliferation. A unitary and analytical overview.

作者信息

Nicolini C

出版信息

Cell Biophys. 1980 Dec;2(4):271-90. doi: 10.1007/BF02785094.

Abstract

The most recent findings on the molecular and cellular characterization of normal and abnormal cell proliferation are summarized. They include molecular spectroscopy, nucleic acid conformation, protein modifications, premature chromosome condensation, nucleoli changes, nuclear and cell morphometry, image analysis, flow microfluorimetry, and time-lapse cinematography. Biophysical and biochemical evidence in favor or against two cycles of chromatin condensation, followed by two abrupt random decondensations, per cell cycle are presented. Other biphasic changes at the molecular and cellular levels that favor the existence of two random transitions, or restriction points, per cell cycle are discussed. A comprehensive unitary model of the cell cycle is then outlined; this model is able to explain most findings on continuously dividing cells and on quiescent cells induced to proliferate. Within this analytical framework the physical-chemical and biological properties are given, in either normal or tumor cells, for the various types of "noncycling" cells that are here viewed as necessary steps in mammalian cell growth rather than separates states. The implications of the coupling of higher-order chromatin structure with cell geometry and growth, high in fibroblast-like cells but low in transformed cells, are also discussed. Molecular mechanisms likely responsible for the chromatin conformational changes occurring at the G0 leads to G1, G1 leads to S, G2 leads to M transitions are finally discussed in terms of polyelectrolyte theory.

摘要

本文总结了关于正常和异常细胞增殖的分子与细胞特征的最新研究发现。这些发现包括分子光谱学、核酸构象、蛋白质修饰、早熟染色体凝聚、核仁变化、细胞核和细胞形态测量、图像分析、流式微量荧光测定法以及延时摄影术。文中展示了支持或反对每个细胞周期中染色质凝聚出现两个周期,随后伴随两次突然随机解聚的生物物理和生化证据。还讨论了分子和细胞水平上其他支持每个细胞周期存在两个随机转变或限制点的双相变化。接着概述了一个全面统一的细胞周期模型;该模型能够解释关于连续分裂细胞以及诱导静止细胞增殖的大多数研究发现。在这个分析框架内,给出了正常或肿瘤细胞中各种类型“非循环”细胞的物理化学和生物学特性,这里将这些细胞视为哺乳动物细胞生长的必要步骤而非单独的状态。还讨论了高阶染色质结构与细胞几何形状和生长之间的耦合关系,这种耦合在成纤维细胞样细胞中较高而在转化细胞中较低。最后根据聚电解质理论讨论了可能导致在G0到G1、G1到S、G2到M转变过程中发生染色质构象变化的分子机制。

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