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伤口修复过程中血管细胞上αVβ3的瞬时功能性表达。

Transient functional expression of alphaVbeta 3 on vascular cells during wound repair.

作者信息

Clark R A, Tonnesen M G, Gailit J, Cheresh D A

机构信息

Department of Dermatology, State University of New York at Stony Brook, 11794-8165, USA.

出版信息

Am J Pathol. 1996 May;148(5):1407-21.

Abstract

During early granulation tissue formation of wound repair, new capillaries invade the fibrin clot, a process that undoubtedly requires an interaction of vascular cells with the wound provisional matrix composed mainly of fibrin, fibronectin, and vitronectin. Integrin alphaVbeta3 is the vascular cell receptor for these wound-associated adhesive proteins. Therefore, we investigated the expression of this receptor on new capillaries of healing full-thickness cutaneous porcine wounds. During granulation tissue formation, alphaVbeta3 was expressed specifically on capillary sprouts invading the central fibrin clot whereas the closely related integrin alphaVbeta5 failed to localize to these cells. Cyclic peptides or antibody antagonists of alphaVbeta3 specifically inhibited granulation tissue formation in a transient manner during the period of invasive angiogenesis. Immunolocalization studies revealed that alphaVbeta3 became aggregated and lost from sprouting vessels after treatment with a peptide antagonist. In contrast, beta 1 integrins were not modulated by this treatment. Once granulation tissue filled the wound and invasive angiogenesis terminated, the alphaVbeta3 showed little or no expression in the granulation tissue microvasculature. These data demonstrate that integrin alphaVbeta3 plays a fundamental, but transient, role during invasive angiogenesis and granulation tissue formation in a healing wound.

摘要

在伤口修复的早期肉芽组织形成过程中,新的毛细血管侵入纤维蛋白凝块,这一过程无疑需要血管细胞与主要由纤维蛋白、纤连蛋白和玻连蛋白组成的伤口临时基质相互作用。整合素αVβ3是这些与伤口相关的黏附蛋白的血管细胞受体。因此,我们研究了该受体在愈合中的猪全层皮肤伤口新毛细血管上的表达。在肉芽组织形成过程中,αVβ3特异性表达于侵入中央纤维蛋白凝块的毛细血管芽上,而密切相关的整合素αVβ5未能定位于这些细胞。αVβ3的环肽或抗体拮抗剂在侵袭性血管生成期间以短暂的方式特异性抑制肉芽组织形成。免疫定位研究显示,用肽拮抗剂处理后,αVβ3从发芽血管中聚集并消失。相比之下,β1整合素不受该处理的调节。一旦肉芽组织填满伤口且侵袭性血管生成终止,αVβ3在肉芽组织微血管中几乎不表达或不表达。这些数据表明,整合素αVβ3在愈合伤口的侵袭性血管生成和肉芽组织形成过程中起重要但短暂的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3348/1861547/a7783eba5594/amjpathol00041-0089-a.jpg

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