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隧道纳米管和相关结构:形成和功能的分子机制。

Tunneling nanotubes and related structures: molecular mechanisms of formation and function.

机构信息

Laboratory of Cellular Dynamics, Regional Centre for Biotechnology, NCR Biotech Science Cluster, 3rd Milestone Faridabad-Gurgaon Expressway, Faridabad, Haryana 121001, India.

Affiliated to the Kalinga Institute of Industrial Technology, Bhubaneswar, Odisha 751024, India.

出版信息

Biochem J. 2021 Nov 26;478(22):3977-3998. doi: 10.1042/BCJ20210077.

Abstract

Tunneling nanotubes (TNTs) are F-actin-based, membrane-enclosed tubular connections between animal cells that transport a variety of cellular cargo. Over the last 15 years since their discovery, TNTs have come to be recognized as key players in normal cell communication and organism development, and are also exploited for the spread of various microbial pathogens and major diseases like cancer and neurodegenerative disorders. TNTs have also been proposed as modalities for disseminating therapeutic drugs between cells. Despite the rapidly expanding and wide-ranging relevance of these structures in both health and disease, there is a glaring dearth of molecular mechanistic knowledge regarding the formation and function of these important but enigmatic structures. A series of fundamental steps are essential for the formation of functional nanotubes. The spatiotemporally controlled and directed modulation of cortical actin dynamics would be required to ensure outward F-actin polymerization. Local plasma membrane deformation to impart negative curvature and membrane addition at a rate commensurate with F-actin polymerization would enable outward TNT elongation. Extrinsic tactic cues, along with cognate intrinsic signaling, would be required to guide and stabilize the elongating TNT towards its intended target, followed by membrane fusion to create a functional TNT. Selected cargoes must be transported between connected cells through the action of molecular motors, before the TNT is retracted or destroyed. This review summarizes the current understanding of the molecular mechanisms regulating these steps, also highlighting areas that deserve future attention.

摘要

隧道纳米管(TNTs)是动物细胞之间基于 F-肌动蛋白的、膜封闭的管状连接,可运输多种细胞货物。自发现以来的过去 15 年中,TNTs 已被认为是正常细胞通讯和生物体发育的关键参与者,并且还被利用来传播各种微生物病原体和主要疾病,如癌症和神经退行性疾病。TNTs 也被提议作为在细胞间传播治疗性药物的方式。尽管这些结构在健康和疾病中的相关性迅速扩展且范围广泛,但对于这些重要而神秘结构的形成和功能的分子机制知识却明显缺乏。功能性纳米管的形成需要一系列基本步骤。需要时空控制和定向调节皮质肌动蛋白动力学,以确保向外的 F-肌动蛋白聚合。局部质膜变形以赋予负曲率,并以与 F-肌动蛋白聚合相称的速度进行膜添加,从而使 TNT 向外伸长。需要外在的策略线索以及同源的内在信号来引导和稳定向外伸长的 TNT 朝向其预期的目标,然后进行膜融合以创建功能性 TNT。选定的货物必须通过分子马达在连接的细胞之间运输,然后 TNT 才能缩回或破坏。本综述总结了调节这些步骤的分子机制的当前理解,还强调了值得未来关注的领域。

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