Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N

Mycobacterium tuberculosis, the causative agent of human tuberculosis, encodes a haemoprotein named Truncated Haemoglobin N (trHbN), which in its active site transforms nitric oxide (NO) to nitrate anion. The NO-dioxygenase activ of trHbN seems to be crucial for the bacillus, which can survive under...

Descripción completa

Guardado en:
Detalles Bibliográficos
Publicado: 2009
Materias:
Ligand migration
Molecular simulations
Mycobacterium tuberculosis
NO detoxification
Truncated haemoglobin N
Acceso en línea:https://bibliotecadigital.exactas.uba.ar/collection/paper/document/paper_18714668_v_n_p33_BidonChanal
http://hdl.handle.net/20.500.12110/paper_18714668_v_n_p33_BidonChanal
Aporte de:
Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA) de Universidad de Buenos Aires
id paper:paper_18714668_v_n_p33_BidonChanal
record_format dspace
spelling paper:paper_18714668_v_n_p33_BidonChanal2023-06-08T16:29:58Z Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N Ligand migration Molecular simulations Mycobacterium tuberculosis NO detoxification Truncated haemoglobin N Mycobacterium tuberculosis Mycobacterium tuberculosis, the causative agent of human tuberculosis, encodes a haemoprotein named Truncated Haemoglobin N (trHbN), which in its active site transforms nitric oxide (NO) to nitrate anion. The NO-dioxygenase activ of trHbN seems to be crucial for the bacillus, which can survive under the nitrosative stress conditions that occur upon infection of the host. As a defense mechanism against the copious amounts of NO produced by macrophages upon infection, the protein must achieve a high level of NO-dioxygenase activ to eliminate NO, but this is modulated by its efficiency in capturing O2 and NO. Migration of small diatomic ligands through the protein matrix is related to the presence of a doubly branched tunnel system connecting the surface and the haem cavsite. In this work, we have studied the mechanism that controls ligand diffusion and product egression with state-of-the-art molecular dynamics simulations. The results support a dual path mechanism for migration of O2 and NO through distinct branches of the tunnel, where migration of NO is facilitated upon binding of O2 to the haem group. Finally, egression of is preceded by the entrance of water to the haem cav and occurs through a different pathway. Overall, the results highlight the intimate relationship between structure, dynamical behavior and biological function of trHbN. © 2009 Springer Netherlands. 2009 https://bibliotecadigital.exactas.uba.ar/collection/paper/document/paper_18714668_v_n_p33_BidonChanal http://hdl.handle.net/20.500.12110/paper_18714668_v_n_p33_BidonChanal
institution Universidad de Buenos Aires
institution_str I-28
repository_str R-134
collection Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA)
topic Ligand migration
Molecular simulations
Mycobacterium tuberculosis
NO detoxification
Truncated haemoglobin N
Mycobacterium tuberculosis
spellingShingle Ligand migration
Molecular simulations
Mycobacterium tuberculosis
NO detoxification
Truncated haemoglobin N
Mycobacterium tuberculosis
Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
topic_facet Ligand migration
Molecular simulations
Mycobacterium tuberculosis
NO detoxification
Truncated haemoglobin N
Mycobacterium tuberculosis
description Mycobacterium tuberculosis, the causative agent of human tuberculosis, encodes a haemoprotein named Truncated Haemoglobin N (trHbN), which in its active site transforms nitric oxide (NO) to nitrate anion. The NO-dioxygenase activ of trHbN seems to be crucial for the bacillus, which can survive under the nitrosative stress conditions that occur upon infection of the host. As a defense mechanism against the copious amounts of NO produced by macrophages upon infection, the protein must achieve a high level of NO-dioxygenase activ to eliminate NO, but this is modulated by its efficiency in capturing O2 and NO. Migration of small diatomic ligands through the protein matrix is related to the presence of a doubly branched tunnel system connecting the surface and the haem cavsite. In this work, we have studied the mechanism that controls ligand diffusion and product egression with state-of-the-art molecular dynamics simulations. The results support a dual path mechanism for migration of O2 and NO through distinct branches of the tunnel, where migration of NO is facilitated upon binding of O2 to the haem group. Finally, egression of is preceded by the entrance of water to the haem cav and occurs through a different pathway. Overall, the results highlight the intimate relationship between structure, dynamical behavior and biological function of trHbN. © 2009 Springer Netherlands.
title Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
title_short Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
title_full Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
title_fullStr Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
title_full_unstemmed Exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin N
title_sort exploring the nitric oxide detoxification mechanism of mycobacterium tuberculosis truncated haemoglobin n
publishDate 2009
url https://bibliotecadigital.exactas.uba.ar/collection/paper/document/paper_18714668_v_n_p33_BidonChanal
http://hdl.handle.net/20.500.12110/paper_18714668_v_n_p33_BidonChanal
_version_ 1768544887347609600

Ejemplares similares