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首页> 外文期刊>The FASEB Journal >Rac1 GTPase silencing counteracts microgravity-induced effects on osteoblastic cells
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Rac1 GTPase silencing counteracts microgravity-induced effects on osteoblastic cells

机译:Rac1 GTPase沉默抵消微重力诱导的对成骨细胞的影响

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摘要

Bone cells exposed to real microgravity display alterations of their cytoskeleton and focal adhesions, two major mechanosensitive structures. These structures are controlled by small GTPases of the Ras homology (Rho) family. We investigated the effects of RhoA, Rac1, and Cdc42 modulation of osteoblastic cells under microgravity conditions. Human MG-63 osteoblastlike cells silenced for RhoGTPases were cultured in the automated Biobox bioreactor (European Space Agency) aboard the Foton M3 satellite and compared to replicate ground-based controls. The cells were fixed after 69 h of microgravity exposure for postflight analysis of focal contacts, F-actin polymerization, vascular endothelial growth factor (VEGF) expression, and matrix targeting. We found that RhoA silencing did not affect sensitivity to microgravity but that Rac1 and, to a lesser extent, Cdc42 abrogation was particularly efficient in counteracting the space-flight-related reduction of the number of focal contacts -50 in silenced, scrambled (SiScr) controls vs. -15 for SiRac1, the number of F-actin fibers (-60 in SiScr controls vs. -10 for SiRac1), and the depletion of matrix-bound VEGF (-40 in SiScr controls vs. -8 for SiRac1). Collectively, these data point out the role of the VEGF/Rho GTPase axis in mechanosensing and validate Rac1-mediated signaling pathways as potential targets for counteracting microgravity effects.
机译:暴露于真实微重力的骨细胞显示出其细胞骨架和黏着斑的改变,这是两种主要的机械敏感结构。这些结构由 Ras 同源 (Rho) 家族的小 GTP 酶控制。我们研究了 RhoA、Rac1 和 Cdc42 调节成骨细胞在微重力条件下的影响。在福田M3卫星上的自动化Biobox生物反应器(欧洲航天局)中培养为RhoGTP酶沉默的人MG-63成骨细胞样细胞,并与重复的地面对照进行比较。在微重力暴露 69 小时后固定细胞,用于黏斑接触、F-肌动蛋白聚合、血管内皮生长因子 (VEGF) 表达和基质靶向的飞行后分析。我们发现 RhoA 沉默不会影响对微重力的敏感性,但 Rac1 和 Cdc42 消除在抵消与空间飞行相关的焦点接触数量减少方面特别有效 [沉默、加扰 (SiScr) 对照组 -50%,SiRac1 组为 -15%),F-肌动蛋白纤维数量(SiScr 对照组为 -60%,SiRac1 组为 -10%), 以及基质结合VEGF的耗竭(SiScr对照组为-40%,SiRac1为-8%)。总的来说,这些数据指出了 VEGF/Rho GTP 酶轴在机械传感中的作用,并验证了 Rac1 介导的信号通路作为抵消微重力效应的潜在靶标。

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