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分离完整的人血浆肽组是一个可以实现的目标吗?

Is isolation of comprehensive human plasma peptidomes an achievable quest?

作者信息

Mahboob S, Mohamedali A, Ahn S B, Schulz-Knappe P, Nice E, Baker M S

机构信息

Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Macquarie University, NSW 2109, Australia.

Department of Chemistry and Biomolecular Sciences, Faculty of Science, Macquarie University, NSW 2109, Australia.

出版信息

J Proteomics. 2015 Sep 8;127(Pt B):300-9. doi: 10.1016/j.jprot.2015.05.010. Epub 2015 May 12.

DOI:10.1016/j.jprot.2015.05.010
PMID:25979773
Abstract

The low molecular weight (LMW; <10kDa)* plasma peptidome has been considered a source of useful diagnostic biomarkers and potentially therapeutic molecules, as it contains many cytokines, peptide hormones, endogenous peptide products and potentially bioactive fragments derived from the parent proteome. The small size of the peptides allows them almost unrestricted vascular and interstitial access, and hence distribution across blood-brain barriers, tumour and other vascular permeability barriers. Therefore, the peptidome may carry specific signatures or fingerprints of an individual's health, wellbeing or disease status. This occurs primarily because of the advantage the peptidome has in being readily accessible in human blood and/or other biofluids. However, the co-expression of highly abundant proteins (>10kDa) and other factors present inherently in human plasma make direct analysis of the blood peptidome one of the most challenging tasks faced in contemporary analytical biochemistry. A comprehensive compendium of extraction and fractionation tools has been collected concerning the isolation and micromanipulation of peptides. However, the search for a reliable, accurate and reproducible single or combinatorial separation process for capturing and analysing the plasma peptidome remains a challenge. This review outlines current techniques used for the separation and detection of plasma peptides and suggests potential avenues for future investigation. This article is part of a Special Issue entitled: HUPO 2014.

摘要

低分子量(LMW;<10kDa)*血浆肽组被认为是有用的诊断生物标志物和潜在治疗分子的来源,因为它包含许多细胞因子、肽类激素、内源性肽产物以及源自母体蛋白质组的潜在生物活性片段。肽的小尺寸使其几乎可以不受限制地进入血管和间质,从而分布于血脑屏障、肿瘤及其他血管通透性屏障。因此,肽组可能携带个体健康、幸福或疾病状态的特定特征或指纹。这主要是因为肽组在人体血液和/或其他生物流体中易于获取。然而,人血浆中固有存在的高丰度蛋白质(>10kDa)和其他因素的共表达,使得直接分析血液肽组成为当代分析生物化学中面临的最具挑战性的任务之一。关于肽的分离和微操作,已经收集了一套全面的提取和分级分离工具。然而,寻找一种可靠、准确且可重复的单一或组合分离方法来捕获和分析血浆肽组仍然是一项挑战。本综述概述了目前用于分离和检测血浆肽的技术,并提出了未来研究的潜在途径。本文是名为:HUPO 2014的特刊的一部分。

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