4.7 Article

Profiling selectivity of chagasin mutants towards cysteine proteases cruzain or cathepsin L through molecular dynamics simulations

期刊

JOURNAL OF BIOMOLECULAR STRUCTURE & DYNAMICS
卷 39, 期 16, 页码 5940-5952

出版社

TAYLOR & FRANCIS INC
DOI: 10.1080/07391102.2020.1796797

关键词

Chagasin; cruzain; cathepsin L; protein-protein interactions; molecular dynamic simulations

资金

  1. CAPES
  2. FAPEMIG
  3. CNPq
  4. CAPES [47/2017, 88881.190367/2018-01]
  5. CNPq researcher fellowship (Bolsa de Produtividade em Pesquisa), level 2

向作者/读者索取更多资源

This study utilized molecular dynamics simulations to investigate the selectivity in inhibition of cruzain or cathepsin L by chagasin mutants W93A, T31A, and T31A/T32A, revealing differences in binding modes and preferences of different mutants, providing insights into their impact on the activities of different enzymes.
Chagasin, an endogenous cysteine protease inhibitor fromTrypanosoma cruzi, can control the activity of the parasitic cruzain and its homologous human cathepsin L. While chagasin inhibits both enzymes with similar potency, mutations have different effects on binding to these enzymes. Mutants T31A and T31A/T32A bind well to cathepsin L, but their affinity for cruzain drops similar to 40 to 140-fold. On the other hand, the mutant W93A binds well to cruzain, but it loses potency against cathepsin L. Here, we employed molecular dynamics simulations to understand the selectivity in inhibition of cruzain or cathepsin L by chagasin mutants W93A, T31A, and T31A/T32A. Our results allowed profiling the nonbonded interactions in the interfaces of each mutant with these cysteine proteases. Additionally, we observed differences in the binding conformation of the chagasin loops L2 and L6 of the W93A mutant, favoring interactions with cruzain and reducing interactions with cathepsin L. These differences are associated with a partial dissociation of the W93A-cathepsin L complex, providing a likely cause for the selectivity of the mutant W93A towards cruzain. Communicated by Ramaswamy H. Sarma.

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