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细胞外基质对血管平滑肌细胞中 RhoA 信号转导的调节作用。

Extracellular matrix effect on RhoA signaling modulation in vascular smooth muscle cells.

机构信息

Department of Systems Biology & Translational Medicine, College of Medicine, Cardiovascular Research Institute, Texas A&M Health Science Center, 336 Reynolds Medical Bldg., College Station, TX 77843-1114, USA.

出版信息

Exp Cell Res. 2010 Oct 15;316(17):2833-48. doi: 10.1016/j.yexcr.2010.06.010. Epub 2010 Jun 16.

Abstract

Morphological adaptations of vascular smooth muscle cells (VSMC) to the mechanically active environment in which they reside, are mediated by direct interactions with the extracellular matrix (ECM) which induces physiological changes at the intracellular level. This study aimed to analyze the effects of the ECM on RhoA-induced mechanical signaling that controls actin organization and focal adhesion formation. VSMC were transfected with RhoA constructs (wild type, dominant negative or constitutively active) and plated on different ECM proteins used as substrate (fibronectin, collagen IV, collagen I, and laminin) or poly-l-lysine as control. Morphological changes of the VSMC were detected by fluorescence confocal microscopy and total internal reflection fluorescence (TIRF) microscopy, and were independently verified using adhesion assays and Western blot analysis. Our results showed that the ECM has an important role in cell spreading, adhesion and morphology with a direct effect on modulating RhoA signaling. RhoA activity significantly affected the stress fibers and focal adhesions reorganization, but in a context imposed by the ECM. Thus, RhoA activity modulation in VSMC induced an increased activation of stress fibers and FA formation at 5h, while a significant inhibition was recorded at 24h after plating on the different ECM. Our findings provide biophysical evidence that ECM modulates VSMC response to mechanical stimuli inducing intracellular biochemical signaling involved in cellular adaptation to the local microenvironment.

摘要

血管平滑肌细胞(VSMC)对其所处的机械活跃环境的形态适应,是通过与细胞外基质(ECM)的直接相互作用来介导的,这种相互作用会在细胞内水平引起生理变化。本研究旨在分析 ECM 对 RhoA 诱导的机械信号的影响,该信号控制着肌动蛋白组织和黏着斑的形成。将 RhoA 构建体(野生型、显性负性或组成性激活)转染到 VSMC 中,并铺在用作底物的不同 ECM 蛋白(纤连蛋白、IV 型胶原、I 型胶原和层粘连蛋白)或聚-l-赖氨酸上或作为对照。通过荧光共焦显微镜和全内反射荧光(TIRF)显微镜检测 VSMC 的形态变化,并通过黏附试验和 Western blot 分析进行独立验证。我们的结果表明,ECM 在细胞铺展、黏附和形态方面具有重要作用,对调节 RhoA 信号具有直接影响。RhoA 活性显著影响应力纤维和黏着斑的重组,但这是在 ECM 施加的背景下发生的。因此,在不同 ECM 上培养 5 小时后,VSMC 中 RhoA 活性的调节会导致应力纤维和 FA 形成的激活增加,而在培养 24 小时后则会显著抑制。我们的发现提供了生物物理证据,表明 ECM 调节 VSMC 对机械刺激的反应,从而诱导涉及细胞对局部微环境适应的细胞内生化信号。

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