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对诱导性收缩环的分析表明蛋白激酶C在胚胎细胞分裂和伤口愈合中发挥作用。

Analysis of inducible contractile rings suggests a role for protein kinase C in embryonic cytokinesis and wound healing.

作者信息

Bement W M, Capco D G

机构信息

Department of Zoology, Arizona State University, Tempe 85287-1501.

出版信息

Cell Motil Cytoskeleton. 1991;20(2):145-57. doi: 10.1002/cm.970200207.

Abstract

A semi-in vitro system derived from Xenopus oocytes which allows induction of contractile ring (CR) formation and closure is described and exploited to elucidate regulatory and structural features of cytokinesis. The inducible CRs (ICRs) are composed of actin filaments and closure is actin filament-dependent as is cytokinesis in vivo. ICR closure in this system is calcium-dependent and pH-sensitive, as is cytokinesis in permeabilized cells (Cande: Journal of Cell Biology 87:326, 1980). Closure of ICRs proceeds at a rate and with a kinetic pattern similar to embryonic cytokinesis. Collectively, these data demonstrate that this system is a faithful mimic of cytokinesis in vivo. ICR formation and closure is protein kinase C (PKC)-dependent and neomycin-sensitive, indicating that the PKC branch of the polyphosphoinositide pathway regulates formation of the actomyosin ring which is the effector of cytokinesis. Kinetic measurements show that the rate of ICR closure reaches a peak of 4-8 microns/sec. Since the maximum measured velocity of actin filament translocation by vertebrate, non-muscle myosins is 0.04 micron/sec, the later observations support a model in which the CR is segmented, containing multiple sites where filaments overlap in a "sliding filament" fashion. Because the rate decreases after reaching a peak, the results also suggest that the number of overlap sites decrease with time.

摘要

本文描述并利用了一种源自非洲爪蟾卵母细胞的半体外系统,该系统可诱导收缩环(CR)的形成与闭合,以阐明胞质分裂的调控和结构特征。可诱导收缩环(ICR)由肌动蛋白丝组成,其闭合依赖于肌动蛋白丝,这与体内的胞质分裂情况相同。在该系统中,ICR的闭合依赖于钙且对pH敏感,这与通透细胞中的胞质分裂情况一致(坎德:《细胞生物学杂志》87:326,1980)。ICR的闭合速率和动力学模式与胚胎胞质分裂相似。总体而言,这些数据表明该系统是体内胞质分裂的忠实模拟。ICR的形成与闭合依赖于蛋白激酶C(PKC)且对新霉素敏感,这表明多磷酸肌醇途径的PKC分支调节着作为胞质分裂效应器的肌动球蛋白环的形成。动力学测量表明,ICR的闭合速率峰值达到4 - 8微米/秒。由于脊椎动物非肌肉肌球蛋白使肌动蛋白丝移位的最大测量速度为0.04微米/秒,后来的观察结果支持了一种模型,即收缩环是分段的,包含多个细丝以“滑动细丝”方式重叠的位点。由于速率在达到峰值后下降,结果还表明重叠位点的数量随时间减少。

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