MptpB, a virulence factor from Mycobacterium tuberculosis, exhibits triple-specificity phosphatase activity

Author:

Beresford Nicola1,Patel Sumayya1,Armstrong Jane2,Szöor Balázs13,Fordham-Skelton Anthony P.2,Tabernero Lydia1

Affiliation:

1. Faculty of Life Sciences, Michael Smith Building, University of Manchester, Manchester M13 9PT, U.K.

2. STFC Daresbury Laboratory, Warrington WA4 4AD, U.K.

3. Institute of Immunology and Infection Research, University of Edinburgh, Edinburgh EH9 3JT, U.K.

Abstract

Bacterial pathogens have developed sophisticated mechanisms of evading the immune system to survive in infected host cells. Central to the pathogenesis of Mycobacterium tuberculosis is the arrest of phagosome maturation, partly through interference with PtdIns signalling. The protein phosphatase MptpB is an essential secreted virulence factor in M. tuberculosis. A combination of bioinformatics analysis, enzyme kinetics and substrate-specificity characterization revealed that MptpB exhibits both dual-specificity protein phosphatase activity and, importantly, phosphoinositide phosphatase activity. Mutagenesis of conserved residues in the active site signature indicates a cysteine-based mechanism of dephosphorylation and identifies two new catalytic residues, Asp165, essential in catalysis, and Lys164, apparently involved in substrate specificity. Sequence similarities with mammalian lipid phosphatases and a preference for phosphoinositide substrates suggests a potential novel role of MptpB in PtdIns metabolism in the host and reveals new perspectives for the role of this phosphatase in mycobacteria pathogenicity.

Publisher

Portland Press Ltd.

Subject

Cell Biology,Molecular Biology,Biochemistry

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