In silico structural characterization of protein targets for drug development against Trypanosoma cruzi |
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| Authors: | Carlyle Ribeiro Lima Nicolas Carels Ana Carolina Ramos Guimaraes Pierre Tufféry Philippe Derreumaux |
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| Affiliation: | 1.Molécules Thérapeutiques in silico,Université Paris Diderot, INSERM UMR-S 973,Paris,France;2.Laboratoire de Biochimie Théorique,CNRS UPR 9080, Institut de Biologie Physico – Chimique, Université Paris Diderot,Paris,France;3.Laboratório de Modelagem de Sistemas Biológicos, National Institute for Science and Technology on Innovation in Neglected Diseases (INCT-IDN), Centro de Desenvolvimento Tecnológico em Saúde (CDTS), Funda??o Oswaldo Cruz (FIOCRUZ),Rio de Janeiro,Brazil;4.Laboratório de Gen?mica Funcional e Bioinformática,Instituto Oswaldo Cruz (IOC), FIOCRUZ,Rio de Janeiro,Brazil |
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| Abstract: | Trypanosoma cruzi is the protozoan pathogen responsible for Chagas disease, which is a major public health problem in tropical and subtropical regions of developing countries and particularly in Brazil. Despite many studies, there is no efficient treatment against Chagas disease, and the search for new therapeutic targets specific to T. cruzi is critical for drug development. Here, we have revisited 41 protein sequences proposed by the analogous enzyme pipeline, and found that it is possible to provide structures for T. cruzi sequences with clear homologs or analogs in H. sapiens and likely associated with trypanothione reductase, cysteine synthase, and ATPase functions, and structures for sequences specific to T. cruzi and absent in H. sapiens associated with 2,4-dienoyl-CoA reductase, and leishmanolysin activities. The implications of our structures refined by atomistic molecular dynamics (monomer or dimer states) in their in vitro environments (aqueous solution or membrane bilayers) are discussed for drug development and suggest that all protein targets, except cysteine synthase, merit further investigation. |
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