Tyrosine Phosphatase MptpA of Mycobacterium Tuberculosis Inhibits Phagocytosis and Increases Actin Polymerization in Macrophages

Overview

Journal Res Microbiol

Publisher Elsevier

Specialty Microbiology

Date 2005 Aug 9

PMID 16085396

Citations 19

Authors

Jerome Castandet

Jean-Francois Prost

Pascale Peyron

Catherine Astarie-Dequeker

Elsa Anes

Alain J Cozzone

Gareth Griffiths

Isabelle Maridonneau-Parini

Affiliations

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Abstract

Protein tyrosine phosphatases from several microorganisms have been shown to play a role as virulence factors by modifying the phosphorylation/dephosphorylation equilibrium in cells of their host. Two tyrosine phosphatases, MptpA and MptpB, secreted by Mycobacterium tuberculosis, have been identified. Expression of MptpA is upregulated upon infection of monocytes, but its role in host cells has not been elucidated. A eukaryotic expression vector containing the mptpA cDNA has been transfected into macrophages. We report that MptpA reduced phagocytosis of mycobacteria, opsonized zymosan or zymosan, but had no effect on phagocytosis of IgG-coated particles. We also noted that the presence of F-actin at the surface of phagosomes containing opsonized zymosan was significantly increased in cells expressing MptpA. In the presence of recombinant MptpA, the process of actin polymerization at the surface of isolated phagosomes was increased; this was not the case in the presence of the phosphatase-dead mutant MptpA(C11S). MptpA had no effect when IgG-coated particles were present inside isolated phagosomes. These results indicate that, like other tyrosine phosphatases of pathogens, MptpA plays a role in phagocytosis and actin polymerization. However, MptpA had no effect on IgG particles, suggesting that its putative substrate(s) is not linked to the signaling pathways of Fcgamma receptors.

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