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神经元轴突中的周期性肌动蛋白结构是维持微管所必需的。

Periodic actin structures in neuronal axons are required to maintain microtubules.

作者信息

Qu Yue, Hahn Ines, Webb Stephen E D, Pearce Simon P, Prokop Andreas

机构信息

Faculty of Biology, Medicine and Health, University of Manchester, Manchester M13 9PT, United Kingdom.

Rutherford Appleton Laboratory, Science and Technology Facilities Council, Didcot OX11 0QX, United Kingdom.

出版信息

Mol Biol Cell. 2017 Jan 15;28(2):296-308. doi: 10.1091/mbc.E16-10-0727. Epub 2016 Nov 23.

Abstract

Axons are cable-like neuronal processes wiring the nervous system. They contain parallel bundles of microtubules as structural backbones, surrounded by regularly spaced actin rings termed the periodic membrane skeleton (PMS). Despite being an evolutionarily conserved, ubiquitous, highly ordered feature of axons, the function of PMS is unknown. Here we studied PMS abundance, organization, and function, combining versatile Drosophila genetics with superresolution microscopy and various functional readouts. Analyses with 11 actin regulators and three actin-targeting drugs suggest that PMS contains short actin filaments that are depolymerization resistant and sensitive to spectrin, adducin, and nucleator deficiency, consistent with microscopy-derived models proposing PMS as specialized cortical actin. Upon actin removal, we observed gaps in microtubule bundles, reduced microtubule polymerization, and reduced axon numbers, suggesting a role of PMS in microtubule organization. These effects become strongly enhanced when carried out in neurons lacking the microtubule-stabilizing protein Short stop (Shot). Combining the aforementioned actin manipulations with Shot deficiency revealed a close correlation between PMS abundance and microtubule regulation, consistent with a model in which PMS-dependent microtubule polymerization contributes to their maintenance in axons. We discuss potential implications of this novel PMS function along axon shafts for axon maintenance and regeneration.

摘要

轴突是连接神经系统的电缆状神经突起。它们包含平行排列的微管束作为结构骨架,周围环绕着规则间隔的肌动蛋白环,称为周期性膜骨架(PMS)。尽管PMS是轴突在进化上保守、普遍存在且高度有序的特征,但其功能尚不清楚。在这里,我们将多种果蝇遗传学方法与超分辨率显微镜以及各种功能读数相结合,研究了PMS的丰度、组织和功能。对11种肌动蛋白调节因子和三种靶向肌动蛋白的药物进行分析表明,PMS包含短肌动蛋白丝,这些丝对解聚具有抗性,并且对血影蛋白、内收蛋白和成核因子缺乏敏感,这与显微镜衍生模型一致,该模型认为PMS是特殊的皮质肌动蛋白。去除肌动蛋白后,我们观察到微管束出现间隙、微管聚合减少以及轴突数量减少,这表明PMS在微管组织中发挥作用。当在缺乏微管稳定蛋白Short stop(Shot)的神经元中进行这些操作时,这些影响会大大增强。将上述肌动蛋白操作与Shot缺乏相结合,揭示了PMS丰度与微管调节之间的密切相关性,这与一个模型一致,即PMS依赖的微管聚合有助于轴突中微管的维持。我们讨论了轴突轴上这种新的PMS功能对轴突维持和再生的潜在影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b2e0/5231898/c46fecaafdc7/296fig1.jpg

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