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内皮细胞管腔和血管引导通道的形成在三维胶原基质中需要MT1-MMP依赖性蛋白水解作用。

Endothelial cell lumen and vascular guidance tunnel formation requires MT1-MMP-dependent proteolysis in 3-dimensional collagen matrices.

作者信息

Stratman Amber N, Saunders W Brian, Sacharidou Anastasia, Koh Wonshill, Fisher Kevin E, Zawieja David C, Davis Michael J, Davis George E

机构信息

Department of Medical Pharmacology and Physiology, School of Medicine, Dalton Cardiovascular Center, University of Missouri-Columbia, MO 65212, USA.

出版信息

Blood. 2009 Jul 9;114(2):237-47. doi: 10.1182/blood-2008-12-196451. Epub 2009 Apr 1.

Abstract

Here we show that endothelial cells (EC) require matrix type 1-metalloproteinase (MT1-MMP) for the formation of lumens and tube networks in 3-dimensional (3D) collagen matrices. A fundamental consequence of EC lumen formation is the generation of vascular guidance tunnels within collagen matrices through an MT1-MMP-dependent proteolytic process. Vascular guidance tunnels represent a conduit for EC motility within these spaces (a newly remodeled 2D matrix surface) to both assemble and remodel tube structures. Interestingly, it appears that twice as many tunnel spaces are created than are occupied by tube networks after several days of culture. After tunnel formation, these spaces represent a 2D migratory surface within 3D collagen matrices allowing for EC migration in an MMP-independent fashion. Blockade of EC lumenogenesis using inhibitors that interfere with the process (eg, integrin, MMP, PKC, Src) completely abrogates the formation of vascular guidance tunnels. Thus, the MT1-MMP-dependent proteolytic process that creates tunnel spaces is directly and functionally coupled to the signaling mechanisms required for EC lumen and tube network formation. In summary, a fundamental and previously unrecognized purpose of EC tube morphogenesis is to create networks of matrix conduits that are necessary for EC migration and tube remodeling events critical to blood vessel assembly.

摘要

在此我们表明,内皮细胞(EC)在三维(3D)胶原基质中形成管腔和管网需要基质金属蛋白酶1(MT1-MMP)。EC管腔形成的一个基本结果是通过MT1-MMP依赖的蛋白水解过程在胶原基质内产生血管引导隧道。血管引导隧道是这些空间(新重塑的二维基质表面)内EC运动的管道,用于组装和重塑管结构。有趣的是,培养几天后,似乎形成的隧道空间数量是管网占据空间数量的两倍。隧道形成后,这些空间代表3D胶原基质内的二维迁移表面,允许EC以MMP非依赖的方式迁移。使用干扰该过程的抑制剂(如整合素、MMP、PKC、Src)阻断EC成管作用,可完全消除血管引导隧道的形成。因此,产生隧道空间的MT1-MMP依赖的蛋白水解过程与EC管腔和管网形成所需的信号传导机制直接且功能上相关联。总之,EC管形态发生的一个基本且以前未被认识到的目的是创建基质管道网络,这些网络对于EC迁移和对血管组装至关重要的管重塑事件是必需的。

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