A computational method for the prediction and functional analysis of potential Mycobacterium tuberculosis adhesin-related proteins.

IF 3.8 3区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS Expert Review of Proteomics Pub Date : 2023-07-01 Epub Date: 2023-12-30 DOI:10.1080/14789450.2023.2275678
Rivesh Maharajh, Manormoney Pillay, Sibusiso Senzani
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Abstract

Objectives: Mycobacterial adherence plays a major role in the establishment of infection within the host. Adhesin-related proteins attach to host receptors and cell-surface components. The current study aimed to utilize in-silico strategies to determine the adhesin potential of conserved hypothetical (CH) proteins.

Methods: Computational analysis was performed on the whole Mycobacterium tuberculosis H37Rv proteome using a software program for the prediction of adhesin and adhesin-like proteins using neural networks (SPAAN) to determine the adhesin potential of CH proteins. A robust pipeline of computational analysis tools: Phyre2 and pFam for homology prediction; Mycosub, PsortB, and Loctree3 for subcellular localization; SignalP-5.0 and SecretomeP-2.0 for secretory prediction, were utilized to identify adhesin candidates.

Results: SPAAN revealed 776 potential adhesins within the whole MTB H37Rv proteome. Comprehensive analysis of the literature was cross-tabulated with SPAAN to verify the adhesin prediction potential of known adhesin (n = 34). However, approximately a third of known adhesins were below the probability of adhesin (Pad) threshold (Pad ≥0.51). Subsequently, 167 CH proteins of interest were categorized using essential in-silico tools.

Conclusion: The use of SPAAN with supporting in-silico tools should be fundamental when identifying novel adhesins. This study provides a pipeline to identify CH proteins as functional adhesin molecules.

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一种用于预测和功能分析潜在结核分枝杆菌粘附素相关蛋白的计算方法。
目的:分枝杆菌的粘附在宿主内感染的建立中起着重要作用。粘附素相关蛋白附着在宿主受体和细胞表面成分上。目前的研究旨在利用计算机策略来确定保守假设(CH)蛋白的粘附素潜力。方法:使用神经网络预测粘附素和粘附素样蛋白的软件程序(SPAAN)对结核分枝杆菌H37Rv的整个蛋白质组进行计算分析,以确定CH蛋白的粘附素潜力。计算分析工具的强大管道:用于同源性预测的Phyre2和pFam;用于亚细胞定位的Mycosub、PsortB和Loctree3;用于分泌预测的SignalP-5.0和SecretomeP-2.0用于鉴定粘附素候选者。结果:SPAAN在整个MTB H37Rv蛋白质组中揭示了776个潜在的粘附素。将文献的综合分析与SPAAN交叉制成表格,以验证已知粘附素(n = 34)。然而,大约三分之一的已知粘连蛋白低于粘连蛋白(Pad)阈值的概率(Pad≥0.51)。随后,使用必要的计算机工具对167种感兴趣的CH蛋白进行了分类。结论:在鉴定新型粘附素时,SPAAN与支持性硅工具的结合应是基础。这项研究为鉴定CH蛋白作为功能性粘附素分子提供了途径。
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来源期刊
Expert Review of Proteomics
Expert Review of Proteomics 生物-生化研究方法
CiteScore
7.60
自引率
0.00%
发文量
20
审稿时长
6-12 weeks
期刊介绍: Expert Review of Proteomics (ISSN 1478-9450) seeks to collect together technologies, methods and discoveries from the field of proteomics to advance scientific understanding of the many varied roles protein expression plays in human health and disease. The journal coverage includes, but is not limited to, overviews of specific technological advances in the development of protein arrays, interaction maps, data archives and biological assays, performance of new technologies and prospects for future drug discovery. The journal adopts the unique Expert Review article format, offering a complete overview of current thinking in a key technology area, research or clinical practice, augmented by the following sections: Expert Opinion - a personal view on the most effective or promising strategies and a clear perspective of future prospects within a realistic timescale Article highlights - an executive summary cutting to the author''s most critical points.
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