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细胞如何(可能)感知微重力。

How cells (might) sense microgravity.

作者信息

Ingber D

机构信息

Departments of Pathology & Surgery, Children's Hospital and Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

FASEB J. 1999;13 Suppl:S3-15. doi: 10.1096/fasebj.13.9001.s3.

Abstract

This article is a summary of a lecture presented at an ESA/NASA Workshop on Cell and Molecular Biology Research in Space that convened in Leuven, Belgium, in June 1998. Recent studies are reviewed which suggest that cells may sense mechanical stresses, including those due to gravity, through changes in the balance of forces that are transmitted across transmembrane adhesion receptors that link the cytoskeleton to the extracellular matrix and to other cells (e.g., integrins, cadherins, selectins). The mechanism by which these mechanical signals are transduced and converted into a biochemical response appears to be based, in part, on the finding that living cells use a tension-dependent form of architecture, known as tensegrity, to organize and stabilize their cytoskeleton. Because of tensegrity, the cellular response to stress differs depending on the level of pre-stress (pre-existing tension) in the cytoskeleton and it involves all three cytoskeletal filament systems as well as nuclear scaffolds. Recent studies confirm that alterations in the cellular force balance can influence intracellular biochemistry within focal adhesion complexes that form at the site of integrin binding as well as gene expression in the nucleus. These results suggest that gravity sensation may not result from direct activation of any single gravioreceptor molecule. Instead, gravitational forces may be experienced by individual cells in the living organism as a result of stress-dependent changes in cell, tissue, or organ structure that, in turn, alter extracellular matrix mechanics, cell shape, cytoskeletal organization, or internal pre-stress in the cell-tissue matrix.--Ingber, D. How cells (might) sense microgravity.

摘要

本文是1998年6月在比利时鲁汶召开的欧洲航天局/美国国家航空航天局空间细胞与分子生物学研究研讨会上一场讲座的总结。本文回顾了近期的研究,这些研究表明,细胞可能通过跨膜粘附受体(将细胞骨架与细胞外基质及其他细胞相连,如整合素、钙粘蛋白、选择素)传递的力平衡变化来感知机械应力,包括重力引起的应力。这些机械信号被转导并转化为生化反应的机制,似乎部分基于以下发现:活细胞利用一种依赖张力的结构形式(称为张拉整体结构)来组织和稳定其细胞骨架。由于张拉整体结构,细胞对应力的反应因细胞骨架中的预应力(预先存在的张力)水平而异,并且涉及所有三种细胞骨架细丝系统以及核支架。近期研究证实,细胞力平衡的改变会影响整合素结合位点形成的粘着斑复合物内的细胞内生化过程以及细胞核中的基因表达。这些结果表明,重力感知可能并非源于任何单个重力受体分子的直接激活。相反,生物体中的单个细胞可能会因细胞、组织或器官结构中依赖应力的变化而感受到引力,这些变化反过来又会改变细胞外基质力学、细胞形状、细胞骨架组织或细胞 - 组织基质中的内部预应力。——英格伯,D. 细胞(可能)如何感知微重力。

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