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斧蛤中极体收缩环的形成与功能。

Formation and function of the polar body contractile ring in Spisula.

作者信息

Pielak Rafal M, Gaysinskaya Valeriya A, Cohen William D

机构信息

Department of Biological Sciences, Hunter College, New York, NY 10021, USA.

出版信息

Dev Biol. 2004 May 15;269(2):421-32. doi: 10.1016/j.ydbio.2004.01.033.

Abstract

Initial studies suggested that spatial organization of the putative polar body contractile ring was determined by the peripheral aster in Spisula [Biol. Bull. 205 (2003) 192]. Here we report detailed supporting observations, including testing of aster and ring function with inhibitors. The metaphase peripheral aster was confirmed to spread cortically in an umbrella-like pattern, with microtubule-poor center. The aster disassembled during anaphase, leaving the spindle docked at the F-actin-poor center of a newly generated cortical F-actin ring that closely approximated the aster in location, measured diameter range, and pattern. Cytochalasin D and latrunculin-B permitted all events except ring and polar body formation. Nocodazole disassembly or taxol stabilization of the peripheral aster produced poorly defined rings or bulging anaphase asters within the ring center, respectively, inhibiting polar body formation. Polar body extrusion occurred at the ring center, the diameter of which diminished. Ring contractility-previously assumed-was verified using blebbistatin, a myosin-II ATPase inhibitor that permitted ring assembly but blocked polar body extrusion. The data support the hypothesis that peripheral aster spreading, perhaps dynein-driven, is causally related to polar body contractile ring formation, with anaphase entry and aster disassembly also required for polar body biogenesis. Previously reported astral spreading during embryonic micromere formation suggests that related mechanisms are involved in asymmetric somatic cytokinesis.

摘要

最初的研究表明,在鸟蛤中,假定的极体收缩环的空间组织是由外周星体决定的[《生物学通报》205 (2003) 192]。在此,我们报告详细的支持性观察结果,包括用抑制剂测试星体和环的功能。中期外周星体被证实以伞状模式在皮质中扩散,中心微管较少。星体在后期解体,纺锤体停靠在新生成的皮质F-肌动蛋白环的F-肌动蛋白较少的中心,该环在位置、测量直径范围和模式上与星体非常接近。细胞松弛素D和拉特肌毒素B允许除环和极体形成之外的所有事件发生。诺考达唑使外周星体解体或用紫杉醇稳定外周星体,分别产生定义不清的环或环中心凸起的后期星体,抑制极体形成。极体挤出发生在环中心,环的直径减小。使用肌球蛋白-II ATP酶抑制剂blebbistatin验证了先前假定的环收缩性,该抑制剂允许环组装但阻止极体挤出。这些数据支持以下假设:外周星体扩散(可能由动力蛋白驱动)与极体收缩环形成存在因果关系,极体生成还需要进入后期和星体解体。先前报道的胚胎小分裂球形成过程中的星体扩散表明,相关机制参与不对称体细胞胞质分裂。

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