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ER sliding dynamics and ER–mitochondrial contacts occur on acetylated microtubules

机译:ER滑动动力学和ER-线粒体接触发生在乙酰化微管上

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摘要

The endoplasmic reticulum (ER) network is extremely dynamic in animal cells, yet little is known about the mechanism and function of its movements. The most common ER dynamic, termed ER sliding, involves ER tubule extension along stable microtubules (MTs). In this study, we show that ER sliding occurs on nocodazole-resistant MTs that are posttranslationally modified by acetylation. We demonstrate that high MT curvature is a good indicator of MT acetylation and show in live cells that ER sliding occurs predominantly on these curved, acetylated MTs. Furthermore, increasing MT acetylation by drug treatment increases the frequency of ER sliding. One purpose of the ER sliding on modified MT tracts could be to regulate its interorganelle contacts. We find that all mitochondria and many endosomes maintain contact with the ER despite the movements of each. However, mitochondria, but not endosomes, preferentially localize to acetylated MTs. Thus, different ER dynamics may occur on distinct MT populations to establish or maintain contacts with different organelles.
机译:内质网(ER)网络在动物细胞中极为活跃,但对其运动的机制和功能知之甚少。最常见的ER动态(称为ER滑动)涉及沿稳定微管(MT)的ER小管延伸。在这项研究中,我们表明内质网滑动发生在耐诺考唑的MTs上,MTs被乙酰化后翻译修饰。我们证明高MT曲率是MT乙酰化的良好指标,并显示在活细胞中ER滑动主要发生在这些弯曲的乙酰化MT上。此外,通过药物治疗增加MT乙酰化会增加ER滑动的频率。 ER在修饰的MT道上滑动的目的之一可能是调节其器官间的接触。我们发现,尽管每个线粒体和许多内体都有运动,但它们仍与ER保持接触。但是,线粒体而不是内体优先定位于乙酰化MTs。因此,不同的ER动态可能会发生在不同的MT群体上,以建立或维持与不同细胞器的接触。

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