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黏附介导的异质性肌动蛋白组织决定凋亡细胞的挤出。

Adhesion-mediated heterogeneous actin organization governs apoptotic cell extrusion.

机构信息

Mechanobiology Institute, National University of Singapore, Singapore, Singapore.

National University of Singapore Graduate School of Integrative Sciences and Engineering, National University of Singapore, Singapore, Singapore.

出版信息

Nat Commun. 2021 Jan 15;12(1):397. doi: 10.1038/s41467-020-20563-9.

Abstract

Apoptotic extrusion is crucial in maintaining epithelial homeostasis. Current literature supports that epithelia respond to extrusion by forming a supracellular actomyosin purse-string in the neighbors. However, whether other actin structures could contribute to extrusion and how forces generated by these structures can be integrated are unknown. Here, we found that during extrusion, a heterogeneous actin network composed of lamellipodia protrusions and discontinuous actomyosin cables, was reorganized in the neighboring cells. The early presence of basal lamellipodia protrusion participated in both basal sealing of the extrusion site and orienting the actomyosin purse-string. The co-existence of these two mechanisms is determined by the interplay between the cell-cell and cell-substrate adhesions. A theoretical model integrates these cellular mechanosensitive components to explain why a dual-mode mechanism, which combines lamellipodia protrusion and purse-string contractility, leads to more efficient extrusion than a single-mode mechanism. In this work, we provide mechanistic insight into extrusion, an essential epithelial homeostasis process.

摘要

细胞凋亡挤出是维持上皮细胞稳态的关键。目前的文献支持上皮细胞通过在相邻细胞中形成超细胞肌动球蛋白束来响应挤出。然而,其他肌动蛋白结构是否可以有助于挤出,以及这些结构产生的力如何被整合,目前还不清楚。在这里,我们发现,在挤出过程中,由片状伪足突起和不连续的肌动球蛋白电缆组成的异质肌动蛋白网络在相邻细胞中重新组织。早期基底片状伪足突起的存在参与了挤出部位的基底密封和肌动球蛋白束的定向。这两种机制的共存取决于细胞-细胞和细胞-基底黏附之间的相互作用。一个理论模型整合了这些细胞机械敏感成分,以解释为什么双模式机制,即结合片状伪足突起和束收缩性,比单模式机制更有效地导致挤出。在这项工作中,我们提供了对挤出这一重要上皮细胞稳态过程的机制见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7467/7810754/a8dab56cb8ef/41467_2020_20563_Fig1_HTML.jpg

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