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静脉和动脉内皮蛋白质组学:挖掘内皮细胞多样性的标志物和机制。

Venous and arterial endothelial proteomics: mining for markers and mechanisms of endothelial diversity.

机构信息

Herman B Wells Center for Pediatric Research, Department of Pediatrics, Indiana University School of Medicine, Indianapolis, IN 46202, USA.

出版信息

Expert Rev Proteomics. 2010 Dec;7(6):823-31. doi: 10.1586/epr.10.92.

Abstract

Endothelial cells (ECs) line the inside of arterial and venous blood vessels in a continuous monolayer and have the important function of responding to environmental cues to regulate vascular tone and new blood vessel formation. They also have well-defined roles in supporting tumorigenesis, and alterations in their function lead to cardiovascular disease. Consequently, ECs have been studied extensively as a cellular model of both normal and abnormal physiology. Despite their importance and the increased utility of proteomic tools in medical research, there are relatively few publications on the topic of vascular endothelial proteomics. A thorough search of the literature mined 52 publications focused exclusively on arterial and/or venous endothelial proteomics. These studies mostly relied upon examination of whole-cell lysates from cultured human umbilical vein ECs to investigate in vitro effects of various molecules, such as VEGF in the context of altering human umbilical vein EC functions related to angiogenesis. Only a few of these publications focused solely on a proteomic characterization of ECs and our analysis further revealed a lack of published studies incorporating proteomic analysis of freshly isolated ECs from tissues or in vitro conditions that mimic in vivo variables, such as oxygen tension and shear stress. It is the purpose of this article to account for the diversity of vascular EC proteomic investigations and comment on the issues that have been and should be addressed in future work.

摘要

内皮细胞(ECs)排列在动脉和静脉血管的内层,形成连续的单层,具有响应环境信号调节血管张力和新血管形成的重要功能。它们在支持肿瘤发生方面也有明确的作用,其功能的改变会导致心血管疾病。因此,ECs 被广泛研究,作为正常和异常生理学的细胞模型。尽管它们很重要,并且蛋白质组学工具在医学研究中的应用越来越多,但关于血管内皮蛋白质组学的出版物相对较少。对文献的全面搜索挖掘出了 52 篇专门针对动脉和/或静脉内皮蛋白质组学的出版物。这些研究主要依赖于培养的人脐静脉内皮细胞的全细胞裂解物来研究各种分子(如 VEGF)的体外作用,以改变与血管生成相关的人脐静脉内皮细胞功能。这些出版物中只有少数专门针对 ECs 的蛋白质组学特征进行了研究,我们的分析还进一步表明,缺乏将蛋白质组学分析整合到从组织或模拟体内变量(如氧张力和切应力)的体外条件下分离的新鲜 ECs 的研究。本文的目的是说明血管内皮细胞蛋白质组学研究的多样性,并对已经和应该在未来工作中解决的问题进行评论。

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