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Leishmania evades host immunity by inhibiting antigen cross-presentation through direct cleavage of the SNARE VAMP8. | LitMetric

AI Article Synopsis

  • Phagocytosis involves immune cells engulfing microorganisms into phagosomes, which then fuse with lysosomes to form phagolysosomes that help kill microbes and present their antigens to T cells via MHC molecules.
  • The parasite Leishmania can evade the immune system by blocking the formation of phagolysosomes through its surface protein GP63, which cleaves SNARE proteins like VAMP8.
  • This disruption prevents necessary changes in phagosome properties and interferes with the presentation of Leishmania antigens, leading to less T cell activation and highlighting the role of VAMP8 in immune response.

Article Abstract

During phagocytosis, microorganisms are taken up by immune cells into phagosomes. Through membrane-trafficking events mediated by SNARE proteins, phagosomes fuse with lysosomes, generating degradative phagolysosomes. Phagolysosomes contribute to host immunity by linking microbial killing within these organelles with antigen processing for presentation on MHC class I or II molecules to T cells. We show that the intracellular parasite Leishmania evades immune recognition by inhibiting phagolysosome biogenesis. The Leishmania cell surface metalloprotease GP63 cleaves a subset of SNAREs, including VAMP8. GP63-mediated VAMP8 inactivation or Vamp8 disruption prevents the NADPH oxidase complex from assembling on phagosomes, thus altering their pH and degradative properties. Consequently, the presentation of exogenous Leishmania antigens on MHC class I molecules, also known as cross-presentation, is inhibited, resulting in reduced T cell activation. These findings indicate that Leishmania subverts immune recognition by altering phagosome function and highlight the importance of VAMP8 in phagosome biogenesis and antigen cross-presentation.

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Source
http://dx.doi.org/10.1016/j.chom.2013.06.003DOI Listing

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