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肌球蛋白XVA亚型参与听觉静纤毛中肌动蛋白细胞骨架的机械转导依赖性重塑。

Myosin XVA isoforms participate in the mechanotransduction-dependent remodeling of the actin cytoskeleton in auditory stereocilia.

作者信息

López-Porras Ana I, Kruse Ava M, McClendon Mark T, Vélez-Ortega A Catalina

出版信息

bioRxiv. 2024 Sep 7:2024.09.04.611210. doi: 10.1101/2024.09.04.611210.

DOI:10.1101/2024.09.04.611210
PMID:39282394
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11398346/
Abstract

Auditory hair cells form precise and sensitive staircase-like actin protrusions known as stereocilia. These specialized microvilli detect deflections induced by sound through the activation of mechano-electrical transduction (MET) channels located at their tips. At rest, a small MET channel current results in a constant calcium influx, which regulates the morphology of the actin cytoskeleton in the shorter 'transducing' stereocilia. However, the molecular mechanisms involved in this novel type of activity-driven plasticity in the stereocilium cytoskeleton are currently unknown. Here, we tested the contribution of myosin XVA (MYO15A) isoforms. We used electron microscopy to evaluate morphological changes in the cytoskeleton of auditory hair cell stereocilia after the pharmacological blockage of resting MET currents in cochlear explants from mice that lacked one or all isoforms of MYO15A. Hair cells lacking functional MYO15A isoforms did not exhibit MET-dependent remodeling in their stereocilia cytoskeleton. In contrast, hair cells that only lack the long isoform of MYO15A exhibited increased MET-dependent stereocilia remodeling, including remodeling in stereocilia from the tallest 'non-transducing' row of the bundle. We conclude that MYO15A isoforms not only enable but also fine-tune the MET-dependent remodeling of the actin cytoskeleton in transducing stereocilia and contribute to the stability of the tallest row.

摘要

听觉毛细胞形成精确且敏感的阶梯状肌动蛋白突起,称为静纤毛。这些特化的微绒毛通过位于其顶端的机械电转导(MET)通道的激活来检测声音引起的偏转。在静息状态下,少量的MET通道电流会导致持续的钙内流,这会调节较短的“转导”静纤毛中肌动蛋白细胞骨架的形态。然而,目前尚不清楚这种新型的活动驱动的静纤毛细胞骨架可塑性所涉及的分子机制。在这里,我们测试了肌球蛋白XVA(MYO15A)异构体的作用。我们使用电子显微镜评估了在缺乏MYO15A一种或所有异构体的小鼠的耳蜗外植体中,静息MET电流被药物阻断后,听觉毛细胞静纤毛细胞骨架的形态变化。缺乏功能性MYO15A异构体的毛细胞在其静纤毛细胞骨架中未表现出MET依赖性重塑。相反,仅缺乏MYO15A长异构体的毛细胞表现出增加的MET依赖性静纤毛重塑,包括来自束中最高的“非转导”排的静纤毛的重塑。我们得出结论,MYO15A异构体不仅能够实现而且还能微调转导静纤毛中肌动蛋白细胞骨架的MET依赖性重塑,并有助于最高排的稳定性。

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