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通过 AQUA 质谱法对高分子量蛋白质平台进行定量分析——以 CD95 诱导死亡信号复合物 (DISC) 为例。

Quantification of High-Molecular Weight Protein Platforms by AQUA Mass Spectrometry as Exemplified for the CD95 Death-Inducing Signaling Complex (DISC).

机构信息

Functional Proteome Analysis, German Cancer Research Center (DKFZ), 69120 Heidelberg, Germany.

Division of Immunogenetics, German Cancer Research Center (DKFZ), 69120 Heidelberg, Germany.

出版信息

Cells. 2013 Jun 27;2(3):476-95. doi: 10.3390/cells2030476.

DOI:10.3390/cells2030476
PMID:24709794
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3972672/
Abstract

Contemporary quantitative mass spectrometry provides fascinating opportunities in defining the stoichiometry of high-molecular weight complexes or multiprotein platforms. The composition stoichiometry of multiprotein platforms is a key to understand the regulation of complex signaling pathways and provides a basis for constructing models in systems biology. Here we present an improved AQUA technique workflow that we adapted for the quantitative mass spectrometry analysis of the stoichiometry of the CD95 (Fas/APO-1) death inducing signaling complex (DISC). The DISC is a high-molecular weight platform essential for the initiation of CD95-mediated apoptotic and non-apoptotic responses. For protein quantification, CD95 DISCs were immunoprecipitated and proteins in the immunoprecipitations were separated by one-dimensional gel electrophoresis, followed by protein quantification using the AQUA technique. We will discuss in detail AQUA analysis of the CD95 DISC focusing on the key issues of this methodology, i.e., selection and validation of AQUA peptides. The application of this powerful method allowed getting new insights into mechanisms of procaspase-8 activation at the DISC and apoptosis initiation [1]. Here we discuss the AQUA methodology adapted by us for the analysis of the CD95 DISC in more detail. This approach paves the way for the successful quantification of multiprotein complexes and thereby delineating the intrinsic details of molecular interactions.

摘要

当代定量质谱技术为定义高分子量复合物或多蛋白平台的化学计量学提供了令人着迷的机会。多蛋白平台的组成化学计量学是理解复杂信号通路调控的关键,并为系统生物学中的构建模型提供了基础。在这里,我们展示了一种改进的 AQUA 技术工作流程,我们将其用于定量质谱分析 CD95(Fas/APO-1)诱导死亡信号复合物(DISC)的化学计量学。DISC 是一个高分子量平台,对于启动 CD95 介导的凋亡和非凋亡反应至关重要。为了进行蛋白质定量,我们使用免疫沉淀法将 CD95 DISC 免疫沉淀,并通过一维凝胶电泳分离免疫沉淀中的蛋白质,然后使用 AQUA 技术进行蛋白质定量。我们将详细讨论 AQUA 分析 CD95 DISC 的方法,重点介绍该方法的关键问题,即 AQUA 肽的选择和验证。这种强大方法的应用使我们能够深入了解 DISC 处 procaspase-8 激活和凋亡起始的机制[1]。在这里,我们将更详细地讨论我们为分析 CD95 DISC 而改编的 AQUA 方法。这种方法为成功定量多蛋白复合物铺平了道路,从而描绘了分子相互作用的内在细节。

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