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人类血小板信号级联的蛋白质组分析。

Proteome analysis of signaling cascades in human platelets.

作者信息

García Angel

机构信息

Oxford Glycobiology Institute, Department of Biochemistry, University of Oxford, South Parks Road, Oxford, OX1 3QU, UK.

出版信息

Blood Cells Mol Dis. 2006 Mar-Apr;36(2):152-6. doi: 10.1016/j.bcmd.2005.12.013. Epub 2006 Feb 17.

Abstract

During the last 15 years, advances in mass spectrometry (MS) instrumentation and techniques have revolutionized the emerging field of proteomics. Proteomics technology allows a comprehensive and efficient analysis of the protein content (i.e., the proteome) of any cell, tissue or biological fluid and has become an indispensable tool in biomedical research, complementing the powerful field of genomics. Proteomics is based on the huge analytical power offered by mass spectrometry in combination with several separation techniques, such as two-dimensional gel electrophoresis (2-DE) or multidimensional liquid chromatography. The technology is particularly suitable for platelets because of the absence of a nucleus. In the recent years, there has been success in mapping the proteome of the platelet in a basal state. Furthermore, a handful of research groups have also applied this technology to the study of signaling cascades in human platelets, allowing the identification of novel platelet signaling proteins and phosphorylation events. Those studies provide new insights into the mechanisms of platelet activation and build the basis for the development of therapeutic agents for thrombotic disease. This article focus on the application of 2-DE-based proteomics to the study of signaling cascades in human platelets.

摘要

在过去的15年里,质谱(MS)仪器和技术的进步彻底改变了新兴的蛋白质组学领域。蛋白质组学技术能够对任何细胞、组织或生物流体中的蛋白质含量(即蛋白质组)进行全面而高效的分析,并且已成为生物医学研究中不可或缺的工具,对强大的基因组学领域起到了补充作用。蛋白质组学基于质谱与多种分离技术(如二维凝胶电泳(2-DE)或多维液相色谱)相结合所提供的巨大分析能力。由于血小板没有细胞核,该技术对血小板特别适用。近年来,已经成功绘制了基础状态下血小板的蛋白质组图谱。此外,一些研究小组也将这项技术应用于人类血小板信号级联的研究,从而能够鉴定新的血小板信号蛋白和磷酸化事件。这些研究为血小板激活机制提供了新的见解,并为血栓性疾病治疗药物的开发奠定了基础。本文重点介绍基于二维凝胶电泳的蛋白质组学在人类血小板信号级联研究中的应用。

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