PtpA, a secreted tyrosine phosphatase from Staphylococcus aureus, contributes to virulence and interacts with coronin-1A during infection

PtpA 是金黄色葡萄球菌分泌的一种酪氨酸磷酸酶,它有助于增强细菌的毒性,并在感染过程中与 coronin-1A 相互作用

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作者:Laila Gannoun-Zaki, Linda Pätzold, Sylvaine Huc-Brandt, Grégory Baronian, Mohamed Ibrahem Elhawy, Rosmarie Gaupp, Marianne Martin, Anne-Béatrice Blanc-Potard, François Letourneur, Markus Bischoff, Virginie Molle

Abstract

Secretion of bacterial signaling proteins and adaptation to the host, especially during infection, are processes that are often linked in pathogenic bacteria. The human pathogen Staphylococcus aureus is equipped with a large arsenal of immune-modulating factors, allowing it to either subvert the host immune response or to create permissive niches for its survival. Recently, we showed that one of the low-molecular-weight protein tyrosine phosphatases produced by S. aureus, PtpA, is secreted during growth. Here, we report that deletion of ptpA in S. aureus affects intramacrophage survival and infectivity. We also observed that PtpA is secreted during macrophage infection. Immunoprecipitation assays identified several host proteins as putative intracellular binding partners for PtpA, including coronin-1A, a cytoskeleton-associated protein that is implicated in a variety of cellular processes. Of note, we demonstrated that coronin-1A is phosphorylated on tyrosine residues upon S. aureus infection and that its phosphorylation profile is linked to PtpA expression. Our results confirm that PtpA has a critical role during infection as a bacterial effector protein that counteracts host defenses.

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