VTR: A Web Tool for Identifying Analogous Contacts on Protein Structures and Their Complexes

VTR: A Web Tool for Identifying Analogous Contacts on Protein Structures and Their Complexes

Evolutionarily related proteins can present similar structures but very dissimilar sequences. Hence, understanding the role of the inter-residues contacts for the protein structure has been the target of many studies. Contacts comprise non-covalent interactions, which are essential to stabilize macr...

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Detalles Bibliográficos
Autores principales: Vitor Pimentel, Diego Mariano, Letícia Xavier Silva Cantão, Luana Luiza Bastos, Pedro Fischer, Leonardo Henrique Franca de Lima, Alexandre Victor Fassio, Raquel Cardoso de Melo-Minardi
Formato: article
Lenguaje:EN
Publicado: Frontiers Media S.A. 2021
Materias:
protein interactions
structural bioinformatics
structural alignment
contacts
rational design of enzymes
Computer applications to medicine. Medical informatics
R858-859.7
Acceso en línea:https://doaj.org/article/48e3df2b9e28426ba537a648ed17e6b3
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Sumario:Evolutionarily related proteins can present similar structures but very dissimilar sequences. Hence, understanding the role of the inter-residues contacts for the protein structure has been the target of many studies. Contacts comprise non-covalent interactions, which are essential to stabilize macromolecular structures such as proteins. Here we show VTR, a new method for the detection of analogous contacts in protein pairs. The VTR web tool performs structural alignment between proteins and detects interactions that occur in similar regions. To evaluate our tool, we proposed three case studies: we 1) compared vertebrate myoglobin and truncated invertebrate hemoglobin; 2) analyzed interactions between the spike protein RBD of SARS-CoV-2 and the cell receptor ACE2; and 3) compared a glucose-tolerant and a non-tolerant β-glucosidase enzyme used for biofuel production. The case studies demonstrate the potential of VTR for the understanding of functional similarities between distantly sequence-related proteins, as well as the exploration of important drug targets and rational design of enzymes for industrial applications. We envision VTR as a promising tool for understanding differences and similarities between homologous proteins with similar 3D structures but different sequences. VTR is available at http://bioinfo.dcc.ufmg.br/vtr.

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