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使用 SEC-MS 方法对拟南芥根膜蛋白组中的蛋白质复合物进行全局鉴定。

Global Identification of Protein Complexes within the Membrane Proteome of Arabidopsis Roots Using a SEC-MS Approach.

机构信息

Department of Plant Systems Biology , Universität Hohenheim , 70593 Stuttgart , Germany.

出版信息

J Proteome Res. 2019 Jan 4;18(1):107-119. doi: 10.1021/acs.jproteome.8b00382. Epub 2018 Nov 13.

Abstract

Biological processes consist of several consecutive and interacting steps as, for example, in signal transduction cascades or metabolic reaction chains. These processes are regulated by protein-protein interactions and the formation of larger protein complexes, which also occur within biological membranes. To gain a large-scale overview of complex-forming proteins and the composition of such complexes within the cellular membranes of Arabidopsis roots, we use the combination of size-exclusion chromatography and mass spectrometry. First, we identified complex-forming proteins by a retention shift analysis relative to expected retention times of monomeric proteins during size-exclusion chromatography. In a second step we predicted complex composition through pairwise correlation of elution profiles. As result we present an interactome of 963 proteins within cellular membranes of Arabidopsis roots. Identification of complex-forming proteins was highly robust between two independently grown root proteomes. The protein complex composition derived from pairwise correlations of coeluting proteins reproducibly identified stable protein complexes (ribosomes, proteasome, mitochondrial respiratory chain supercomplexes) but showed higher variance between replicates regarding transient interactions (e.g., interactions with kinases) within membrane protein complexes.

摘要

生物过程由几个连续且相互作用的步骤组成,例如信号转导级联或代谢反应链。这些过程受蛋白质-蛋白质相互作用和较大蛋白质复合物的形成调控,而这些过程也发生在生物膜内。为了全面了解拟南芥根细胞膜内形成复合物的蛋白质及其复合物的组成,我们使用凝胶过滤色谱和质谱联用的方法。首先,我们通过相对单体蛋白在凝胶过滤色谱中的预期保留时间的保留时间偏移分析来鉴定形成复合物的蛋白质。在第二步中,我们通过洗脱曲线的两两相关性预测复合物组成。结果,我们呈现了拟南芥根细胞膜内 963 种蛋白质的相互作用组。在两个独立生长的根蛋白组之间,形成复合物的蛋白质的鉴定高度稳健。通过共洗脱蛋白的两两相关性得出的蛋白质复合物组成可重现鉴定稳定的蛋白质复合物(核糖体、蛋白酶体、线粒体呼吸链超级复合物),但在膜蛋白复合物内的瞬时相互作用(例如与激酶的相互作用)方面,各重复之间的差异较大。

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