Key allosteric and active site residues of SARS-CoV-2 3CLpro are promising drug targets

Al Adem Kenana; Ferreira Juliana C.; Fadl SamarMustafa MoradRabeh Wael M.

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Key allosteric and active site residues of SARS-CoV-2 3CLpro are promising drug targets

机译：Key allosteric and active site residues of SARS-CoV-2 3CLpro are promising drug targets

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The main protease of SARS-CoV-2, 3-chymotrypsin-like protease (3CLpro), is a prominent target for antiviral development due to its essential role in the viral life cycle. Research has largely focused on competitive inhibitors of 3CLpro that target the active site. However, allosteric sites distal to the peptide substrate-binding region are also potential targets for the design of reversible noncompetitive inhibitors. Computational analyses have examined the importance of key contacts at allosteric sites of 3CLpro, but these contacts have not been validated experimentally. In this work, four druggable pockets spanning the surface of SARS-CoV-2 3CLpro were predicted: pocket 1 is the active site, whereas pockets 2, 3 and 4 are located away from the active site at the interface of domains II and III. Site-directed alanine mutagenesis of selected residues with important structural interactions revealed that 7 of 13 active site residues (N28, R40, Y54, S147, Y161, D187 and Q192) and 7 of 12 allosteric site residues (T111, R131, N133, D197, N203, D289 and D295) are essential for maintaining catalytically active and thermodynamically stable 3CLpro. Alanine substitution at these key amino acid residues inactivated or reduced the activity of 3CLpro. In addition, the thermodynamic stability of 3CLpro decreased in the presence of some of these mutations. This work provides experimental validation of essential contacts in the active and allosteric sites of 3CLpro that could be targeted with competitive and noncompetitive inhibitors as new therapeutics against COVID-19.

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来源
《The Biochemical Journal》 |2023年第11期|791-813|共23页
作者
Al Adem Kenana; Ferreira Juliana C.; Fadl SamarMustafa MoradRabeh Wael M.;
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作者单位

New York Univ Abu Dhabi;

Al Zaytoonah Univ Jordan;

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原文格式 PDF
正文语种英语
中图分类生物化学;
关键词
COV MAIN PROTEASE; MOLECULAR-DYNAMICS; BINDING-SITES; M-PRO; SARS; INHIBITORS; PEPTIDOMIMETICS; DIMERIZATION; PARAMETERS; ACCURACY;

Key allosteric and active site residues of SARS-CoV-2 3CLpro are promising drug targets

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