结核分枝杆菌中广泛存在的腺苷核苷酸结合的鉴定。
Identification of widespread adenosine nucleotide binding in Mycobacterium tuberculosis.
作者信息
Ansong Charles, Ortega Corrie, Payne Samuel H, Haft Daniel H, Chauvignè-Hines Lacie M, Lewis Michael P, Ollodart Anja R, Purvine Samuel O, Shukla Anil K, Fortuin Suereta, Smith Richard D, Adkins Joshua N, Grundner Christoph, Wright Aaron T
机构信息
Biological Sciences Division, Pacific Northwest National Laboratory, Richland, WA 99352, USA.
出版信息
Chem Biol. 2013 Jan 24;20(1):123-33. doi: 10.1016/j.chembiol.2012.11.008.
Abstract
Computational prediction of protein function is frequently error-prone and incomplete. In Mycobacterium tuberculosis (Mtb), ~25% of all genes have no predicted function and are annotated as hypothetical proteins, severely limiting our understanding of Mtb pathogenicity. Here, we utilize a high-throughput quantitative activity-based protein profiling (ABPP) platform to probe, annotate, and validate ATP-binding proteins in Mtb. We experimentally validate prior in silico predictions of >240 proteins and identify 72 hypothetical proteins as ATP binders. ATP interacts with proteins with diverse and unrelated sequences, providing an expanded view of adenosine nucleotide binding in Mtb. Several hypothetical ATP binders are essential or taxonomically limited, suggesting specialized functions in mycobacterial physiology and pathogenicity.
摘要
蛋白质功能的计算预测常常容易出错且不完整。在结核分枝杆菌(Mtb)中,所有基因中约25%没有预测功能,被注释为假设蛋白,这严重限制了我们对Mtb致病性的理解。在此,我们利用基于活性的高通量定量蛋白质谱分析(ABPP)平台来探测、注释和验证Mtb中的ATP结合蛋白。我们通过实验验证了之前对240多种蛋白质的计算机模拟预测,并鉴定出72种假设蛋白为ATP结合蛋白。ATP与具有不同且不相关序列的蛋白质相互作用,这为Mtb中腺苷核苷酸结合提供了更广泛的视角。几种假设的ATP结合蛋白是必需的或在分类学上受到限制,表明它们在分枝杆菌生理学和致病性中具有特殊功能。
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