Mycobacterium tuberculosis ArfA Rv0899

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== Disease ==
== Disease ==
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Rv0899 has been proposed to act as an outer membrane [[porin]] and to contribute to the bacterium's adaptation to the acidic environment of the phagosome[http://en.wikipedia.org/wiki/Phagosome] during infection. The amino acid pair Asn111-Gly112,located at the end of α1 and preceding L3, undergoes in-vitro deamidation, a pH-dependent
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Tuberculosis (TB) is the seventh most common cause of death globally (1). Mycobacterium
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tuberculosis, its causative agent, has achieved a spread in the human population unmatched by
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any other bacterial pathogen (2), despite the availability of effective short-course chemotherapy
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and the Bacille Calmette-Guerin vaccine. Important factors contributing to the high
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pathogenicity of M. tuberculosis are its highly impermeable cell wall, which prevents the
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Rv0899 has been proposed to act as an outer membrane [[porin]] and to contribute to the bacterium's adaptation to the acidic environment of the phagosome[http://en.wikipedia.org/wiki/Phagosome] during infection.uptake of most hydrophilic antibiotic drugs, and its high adaptability to environmental changes
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during the course of infection, including: nutrient deprivation, hypoxia, various exogenous
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stress conditions and the phagosomal environment (3).
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The complete genome sequence of M. tuberculosis H37Rv, the best-characterized strain of the
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bacterium, has identified several stress response genes which contribute to pathogenicity (4).
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Among these, the membrane protein Rv0899, encoded by the rv0899 gene, is thought to confer
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adaptation of M. tuberculosis to the acidic environment of the phagosome (5). Sequence
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analysis of the mycobacterial genomes shows that the gene is restricted to pathogenic
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mycobacteria associated with TB (M. tuberculosis, M. bovis) and other TB-related diseases
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(M. marinum, M. ulcerans, M. kansaii) and, thus, is an attractive candidate for the development
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of anti-TB chemotherapeutic agents. Notably, two M. tuberculosis H37Rv genes (Rv0900 and
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Rv0901) adjacent to Rv0899 also encode putative membrane proteins, and are found
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exclusively in association with Rv0899 in the same pathogenic mycobacteria, suggesting that
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the three may constitute an operon dedicated to a common function
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The amino acid pair Asn111-Gly112,located at the end of α1 and preceding L3, undergoes in-vitro deamidation, a pH-dependent
reaction whereby Asn is converted to Asp and ammonia is released. Asparagine residues
reaction whereby Asn is converted to Asp and ammonia is released. Asparagine residues
preceding glycine, and situated in conformationally flexible regions of proteins, are frequently deamidated, with potentially significant consequences for protein regulation and function
preceding glycine, and situated in conformationally flexible regions of proteins, are frequently deamidated, with potentially significant consequences for protein regulation and function

Revision as of 14:03, 12 January 2015

NMR structure of uncharacterized protein Rv0899 (PDB code 2l26)

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Proteopedia Page Contributors and Editors (what is this?)

Liliya Karasik, Jaime Prilusky, Michal Harel

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