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      An exosome-based secretion pathway is responsible for protein export from Leishmania and communication with macrophages.

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          Abstract

          Specialized secretion systems are used by numerous bacterial pathogens to export virulence factors into host target cells. Leishmania and other eukaryotic intracellular pathogens also deliver effector proteins into host cells; however, the mechanisms involved have remained elusive. In this report, we identify exosome-based secretion as a general mechanism for protein secretion by Leishmania, and show that exosomes are involved in the delivery of proteins into host target cells. Comparative quantitative proteomics unambiguously identified 329 proteins in Leishmania exosomes, accounting for >52% of global protein secretion from these organisms. Our findings demonstrate that infection-like stressors (37 degrees C +/- pH 5.5) upregulated exosome release more than twofold and also modified exosome protein composition. Leishmania exosomes and exosomal proteins were detected in the cytosolic compartment of infected macrophages and incubation of macrophages with exosomes selectively induced secretion of IL-8, but not TNF-alpha. We thus provide evidence for an apparently broad-based mechanism of protein export by Leishmania. Moreover, we describe a mechanism for the direct delivery of Leishmania molecules into macrophages. These findings suggest that, like mammalian exosomes, Leishmania exosomes function in long-range communication and immune modulation.

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          Author and article information

          Journal
          J Cell Sci
          Journal of cell science
          The Company of Biologists
          1477-9137
          0021-9533
          Mar 15 2010
          : 123
          : Pt 6
          Affiliations
          [1 ] Department of Medicine, Division of Infectious Diseases, University of British Columbia, Faculties of Medicine and Science, 2733 Heather St, Vancouver, BC V5Z 3J5, Canada.
          Article
          jcs.056465
          10.1242/jcs.056465
          20159964
          8d00aa28-762d-4855-9b44-c88401caf1ff
          History

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