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整合素结合和机械张力诱导mRNA和核糖体向黏着斑移动。

Integrin binding and mechanical tension induce movement of mRNA and ribosomes to focal adhesions.

作者信息

Chicurel M E, Singer R H, Meyer C J, Ingber D E

机构信息

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

出版信息

Nature. 1998 Apr 16;392(6677):730-3. doi: 10.1038/33719.

Abstract

The extracellular matrix (ECM) activates signalling pathways that control cell behaviour by binding to cell-surface integrin receptors and inducing the formation of focal adhesion complexes (FACs). In addition to clustered integrins, FACs contain proteins that mechanically couple the integrins to the cytoskeleton and to immobilized signal-transducing molecules. Cell adhesion to the ECM also induces a rapid increase in the translation of preexisting messenger RNAs. Gene expression can be controlled locally by targeting mRNAs to specialized cytoskeletal domains. Here we investigate whether cell binding to the ECM promotes formation of a cytoskeletal microcompartment specialized for translational control at the site of integrin binding. High-resolution in situ hybridization revealed that mRNA and ribosomes rapidly and specifically localized to FACs that form when cells bind to ECM-coated microbeads. Relocation of these protein synthesis components to the FAC depended on the ability of integrins to mechanically couple the ECM to the contractile cytoskeleton and on associated tension-moulding of the actin lattice. Our results suggest a new type of gene regulation by integrins and by mechanical stress which may involve translation of mRNAs into proteins near the sites of signal reception.

摘要

细胞外基质(ECM)通过与细胞表面整合素受体结合并诱导粘着斑复合物(FACs)的形成来激活控制细胞行为的信号通路。除了聚集的整合素外,粘着斑复合物还包含将整合素与细胞骨架和固定的信号转导分子机械连接的蛋白质。细胞与细胞外基质的粘附还会导致已有信使核糖核酸(mRNA)的翻译迅速增加。基因表达可以通过将mRNA靶向特定的细胞骨架结构域进行局部控制。在这里,我们研究细胞与细胞外基质的结合是否会促进在整合素结合位点形成专门用于翻译控制的细胞骨架微区室。高分辨率原位杂交显示,当细胞与包被有细胞外基质的微珠结合时,mRNA和核糖体迅速且特异性地定位于形成的粘着斑复合物。这些蛋白质合成成分重新定位于粘着斑复合物取决于整合素将细胞外基质与收缩性细胞骨架机械连接的能力以及肌动蛋白晶格相关的张力塑造。我们的结果表明整合素和机械应力可能涉及一种新型的基因调控,这可能包括在信号接收位点附近将mRNA翻译成蛋白质。

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