Título
Identification of the NADP+ structural binding site and coenzyme effect on the fused G6PD::6PGL protein from Giardia lamblia
Autor
Roberto Arreguin
Yudibeth Sixto-López
NOEMI CARDENAS-RODRIGUEZ
Rosa Angélica Castillo-Rodríguez
Daniel Ortega-Cuellar
Nivel de Acceso
Acceso Abierto
Materias
BIOLOGÍA Y QUÍMICA - (CTI) NADP + structural binding site - ([Biomolecules (eISSN: 2218-273X) 10, 46]) Stability - ([Biomolecules (eISSN: 2218-273X) 10, 46]) 6GPD - ([Biomolecules (eISSN: 2218-273X) 10, 46]) Docking - ([Biomolecules (eISSN: 2218-273X) 10, 46]) Giardia lamblia - ([Biomolecules (eISSN: 2218-273X) 10, 46])
Resumen o descripción
Giardia lambia is a flagellated protozoan parasite that lives in the small intestine and is the causal agent of giardiasis. It has been reported that G. lamblia exhibits glucose-6-phosphate dehydrogenase (G6PD), the first enzyme in the pentose phosphate pathway (PPP). Our group work demonstrated that the g6pd and 6pgl genes are present in the open frame that gives rise to the fused G6PD::6PGL protein; where the G6PD region is similar to the 3D structure of G6PD in Homo sapiens. The objective of the present work was to show the presence of the structural NADP(+) binding site on the fused G6PD::6PGL protein and evaluate the effect of the NADP(+) molecule on protein stability using biochemical and computational analysis. A protective effect was observed on the thermal inactivation, thermal stability, and trypsin digestions assays when the protein was incubated with NADP(+). By molecular docking, we determined the possible structural-NADP(+) binding site, which is located between the Rossmann fold of G6PD and 6PGL. Finally, molecular dynamic (MD) simulation was used to test the stability of this complex; it was determined that the presence of both NADP(+) structural and cofactor increased the stability of the enzyme, which is in agreement with our experimental results.
Fecha de publicación
2020
Tipo de publicación
Artículo
https://doi.org/10.3390/biom10010046
Recurso de información
Formato
application/pdf
Fuente
Biomolecules (eISSN: 2218-273X) 10, 46
Idioma
Inglés
Relación
https://www.mdpi.com/journal/biomolecules
Repositorio Orígen
Repositorio del Instituto de Química
Descargas
0