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中心粒微管三联体的延长有助于γ-微管蛋白缺失细胞中有丝分裂纺锤体的形成。

Elongation of centriolar microtubule triplets contributes to the formation of the mitotic spindle in gamma-tubulin-depleted cells.

作者信息

Raynaud-Messina Brigitte, Mazzolini Laurent, Moisand André, Cirinesi Anne-Marie, Wright Michel

机构信息

ISTMT, Centre de Recherche en Pharmacologie-Santé, UMR 2587 CNRS-P. Fabre, 3 rue des Satellites, 31 400 Toulouse, France.

出版信息

J Cell Sci. 2004 Nov 1;117(Pt 23):5497-507. doi: 10.1242/jcs.01401. Epub 2004 Oct 12.

Abstract

The assembly of the mitotic spindle after depletion of the major gamma-tubulin isotype by RNA-mediated interference was assessed in the Drosophila S2 cell line. Depletion of gamma-tubulin had no significant effect on the cytoskeletal microtubules during interphase. However, it promoted an increase in the mitotic index, resulting mainly in monopolar and, to a lesser extent, asymmetrical bipolar prometaphases lacking astral microtubules. This mitotic accumulation coincided with the activation of the mitotic checkpoint. Immunostaining with an anti-Asp antibody revealed that the spindle poles, which were always devoid of gamma-tubulin, were unfocused and organized into sub-spindles. Despite the marked depletion of gamma-tubulin, the pericentriolar proteins CP190 and centrosomin were recruited to the spindle pole(s), where they formed three or four dots, suggesting the presence of several centrioles. Electron microscopic reconstructions demonstrated that most of the monopolar spindles exhibited three or four centrioles, indicating centriole duplication with a failure in the separation process. Most of the centrioles were shortened, suggesting a role for gamma-tubulin in centriole morphogenesis. Moreover, in contrast to metaphases observed in control cells, in which the spindle microtubules radiated from the pericentriolar material, in gamma-tubulin-depleted cells, microtubule assembly still occurred at the poles but involved the elongation of centriolar microtubule triplets. Our results demonstrate that, after depletion of gamma-tubulin, the pericentriolar material is unable to promote efficient microtubule nucleation. They point to an alternative mechanism of centrosomal microtubule assembly that contributes to the formation of abnormal, albeit partially functional, mitotic spindles.

摘要

通过RNA介导的干扰耗尽主要的γ-微管蛋白同种型后,在果蝇S2细胞系中评估有丝分裂纺锤体的组装。γ-微管蛋白的耗尽在间期对细胞骨架微管没有显著影响。然而,它促进了有丝分裂指数的增加,主要导致单极,并且在较小程度上导致缺乏星体微管的不对称双极前中期。这种有丝分裂积累与有丝分裂检查点的激活同时发生。用抗Asp抗体进行免疫染色显示,总是缺乏γ-微管蛋白的纺锤体极未聚焦并组织成亚纺锤体。尽管γ-微管蛋白明显耗尽,但中心粒周围蛋白CP190和中心体蛋白被募集到纺锤体极,在那里它们形成三到四个点,表明存在几个中心粒。电子显微镜重建表明,大多数单极纺锤体显示三或四个中心粒,表明中心粒复制但分离过程失败。大多数中心粒缩短,表明γ-微管蛋白在中心粒形态发生中起作用。此外,与对照细胞中观察到的中期不同,对照细胞中的纺锤体微管从中心粒周围物质辐射出来,在γ-微管蛋白耗尽的细胞中,微管组装仍在极处发生,但涉及中心粒微管三联体的延长。我们的结果表明,γ-微管蛋白耗尽后,中心粒周围物质无法促进有效的微管成核。它们指出了一种中心体微管组装的替代机制,这种机制有助于形成异常但部分功能正常的有丝分裂纺锤体。

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