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α5和αv整合素在体内协同调节血管平滑肌和神经嵴功能。

α5 and αv integrins cooperate to regulate vascular smooth muscle and neural crest functions in vivo.

作者信息

Turner Christopher J, Badu-Nkansah Kwabena, Crowley Denise, van der Flier Arjan, Hynes Richard O

机构信息

Howard Hughes Medical Institute, Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

Howard Hughes Medical Institute, Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA

出版信息

Development. 2015 Feb 15;142(4):797-808. doi: 10.1242/dev.117572.

Abstract

The RGD-binding α5 and αv integrins have been shown to be key regulators of vascular smooth muscle cell (vSMC) function in vitro. However, their role on vSMCs during vascular development in vivo remains unclear. To address this issue, we have generated mice that lack α5, αv or both α5 and αv integrins on their vSMCs, using the SM22α-Cre transgenic mouse line. To our surprise, neither α5 nor αv mutants displayed any obvious vascular defects during embryonic development. By contrast, mice lacking both α5 and αv integrins developed interrupted aortic arches, large brachiocephalic/carotid artery aneurysms and cardiac septation defects, but developed extensive and apparently normal vasculature in the skin. Cardiovascular defects were also found, along with cleft palates and ectopically located thymi, in Wnt1-Cre α5/αv mutants, suggesting that α5 and αv cooperate on neural crest-derived cells to control the remodelling of the pharyngeal arches and the septation of the heart and outflow tract. Analysis of cultured α5/αv-deficient vSMCs suggests that this is achieved, at least in part, through proper assembly of RGD-containing extracellular matrix proteins and the correct incorporation and activation of latent TGF-β.

摘要

RGD结合性α5和αv整合素已被证明是体外血管平滑肌细胞(vSMC)功能的关键调节因子。然而,它们在体内血管发育过程中对vSMC的作用仍不清楚。为了解决这个问题,我们利用SM22α-Cre转基因小鼠品系,培育出了vSMC上缺乏α5、αv或同时缺乏α5和αv整合素的小鼠。令我们惊讶的是,α5和αv突变体在胚胎发育过程中均未表现出任何明显的血管缺陷。相比之下,同时缺乏α5和αv整合素的小鼠出现了主动脉弓中断、头臂/颈动脉大动脉瘤和心脏间隔缺损,但皮肤中却发育出了广泛且明显正常的脉管系统。在Wnt1-Cre α5/αv突变体中还发现了心血管缺陷,以及腭裂和异位胸腺,这表明α5和αv在神经嵴衍生细胞上协同作用,以控制咽弓的重塑以及心脏和流出道的分隔。对培养的α5/αv缺陷型vSMC的分析表明,这至少部分是通过含RGD的细胞外基质蛋白的正确组装以及潜伏性TGF-β的正确掺入和激活来实现的。

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