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一种肽组学策略,旨在阐明使肽类激素失活的蛋白水解途径。

A peptidomics strategy to elucidate the proteolytic pathways that inactivate peptide hormones.

机构信息

Department of Chemistry and Chemical Biology, Harvard University, 12 Oxford Street, Cambridge, Massachusetts 02138, United States.

出版信息

Biochemistry. 2011 Mar 29;50(12):2213-22. doi: 10.1021/bi2000033. Epub 2011 Feb 22.

Abstract

Proteolysis plays a key role in regulating the levels and activity of peptide hormones. Characterization of the proteolytic pathways that cleave peptide hormones is of basic interest and can, in some cases, spur the development of novel therapeutics. The lack, however, of an efficient approach to identify endogenous fragments of peptide hormones has hindered the elucidation of these proteolytic pathways. Here, we apply a mass spectrometry (MS) based peptidomics approach to characterize the intestinal fragments of peptide histidine isoleucine (PHI), a hormone that promotes glucose-stimulated insulin secretion (GSIS). Our approach reveals a proteolytic pathway in the intestine that truncates PHI at its C-terminus to produce a PHI fragment that is inactive in a GSIS assay, a result that provides a potential mechanism of PHI regulation in vivo. Differences between these in vivo peptidomics studies and in vitro lysate experiments, which showed N- and C-terminal processing of PHI, underscore the effectiveness of this approach to discover physiologically relevant proteolytic pathways. Moreover, integrating this peptidomics approach with bioassays (i.e., GSIS) provides a general strategy to reveal proteolytic pathways that may regulate the activity of peptide hormones.

摘要

蛋白水解在调节肽激素的水平和活性方面起着关键作用。鉴定切割肽激素的蛋白水解途径具有基础意义,在某些情况下可以促进新型治疗药物的开发。然而,缺乏一种有效的方法来识别内源性肽激素片段,这阻碍了这些蛋白水解途径的阐明。在这里,我们应用基于质谱 (MS) 的肽组学方法来研究促进葡萄糖刺激胰岛素分泌 (GSIS) 的激素——组氨酸异亮氨酸肽 (PHI) 的肠道片段。我们的方法揭示了一种在肠道中截断 PHI 的 C 末端的蛋白水解途径,产生一种在 GSIS 测定中无活性的 PHI 片段,这一结果为 PHI 体内调节提供了一个潜在的机制。这些体内肽组学研究与体外溶胞产物实验之间的差异,表明 PHI 的 N 端和 C 端加工,突显了这种方法发现与生理相关的蛋白水解途径的有效性。此外,将这种肽组学方法与生物测定(即 GSIS)相结合,提供了一种揭示可能调节肽激素活性的蛋白水解途径的通用策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f43e/3076939/c6a5f95f443c/nihms272070f1.jpg

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