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中心体稳态中的微管马达:癌症治疗的新靶点?

Microtubule motors in centrosome homeostasis: A target for cancer therapy?

机构信息

Cellular Dyshomeostasis Laboratory (CDHL), School of Chemical and Bio Technology, SASTRA University, Thanjavur 613 401, Tamil Nadu, India.

Cellular Dyshomeostasis Laboratory (CDHL), School of Chemical and Bio Technology, SASTRA University, Thanjavur 613 401, Tamil Nadu, India.

出版信息

Biochim Biophys Acta Rev Cancer. 2021 Apr;1875(2):188524. doi: 10.1016/j.bbcan.2021.188524. Epub 2021 Feb 12.

Abstract

Cancer is a grievous concern to human health, owing to a massive heterogeneity in its cause and impact. Dysregulation (numerical, positional and/or structural) of centrosomes is one of the notable factors among those that promote onset and progression of cancers. In a normal dividing cell, a pair of centrosomes forms two poles, thereby governing the formation of a bipolar spindle assembly. A large number of cancer cells, however, harbor supernumerary centrosomes, which mimic the bipolar arrangement in normal cells by centrosome clustering (CC) into two opposite poles, thus developing a pseudo-bipolar spindle assembly. Manipulation of centrosome homeostasis is the paramount pre-requisite for the evasive strategy of CC in cancers. Out of the varied factors that uphold centrosome integrity, microtubule motors (MiMos) play a critical role. Categorized as dyneins and kinesins, MiMos are involved in cohesion of centrosomes, and also facilitate the maintenance of the numerical, positional and structural integrity of centrosomes. Herein, we elucidate the decisive mechanisms undertaken by MiMos to mediate centrosome homeostasis, and how dysregulation of the same might lead to CC in cancer cells. Understanding the impact of MiMos on CC might open up avenues toward a credible therapeutic target against diverse cancers.

摘要

癌症是人类健康的严重隐患,其病因和影响存在巨大的异质性。中心体的失调(数量、位置和/或结构)是促进癌症发生和发展的显著因素之一。在正常分裂的细胞中,一对中心体形成两个极,从而控制双极纺锤体的形成。然而,大量癌细胞拥有多余的中心体,通过中心体聚集(CC)形成两个相对的极,模拟正常细胞的双极排列,从而形成伪双极纺锤体。操纵中心体稳态是 CC 在癌症中逃避策略的首要前提。在维持中心体完整性的各种因素中,微管马达(MiMos)起着关键作用。MiMos 分为驱动蛋白和动力蛋白,参与中心体的黏合,并有助于维持中心体的数量、位置和结构完整性。本文阐述了 MiMos 介导中心体稳态的决定性机制,以及同一机制的失调如何导致癌细胞的 CC。了解 MiMos 对 CC 的影响可能为针对多种癌症的可信治疗靶点开辟途径。

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