ausblenden:
Schlagwörter:
-
Zusammenfassung:
Immune cell phenotyping frequently detects lineage -unrelated receptors. Here, we report that surface receptors can be transferred from primary macrophages to CD4 T cells and identify the Fcy receptor CD32 as driver and cargo of this trogocytotic transfer. Filamentous CD32 + nanoprotrusions deposit distinct plasma membrane patches onto target T cells. Transferred receptors confer cell migration and adhesion properties, and macrophage -derived membrane patches render resting CD4 T cells susceptible to infection by serving as hotspots for HIV -1 binding. Antibodies that recognize T cell epitopes enhance CD32-mediated trogocytosis. Such autoreactive anti -HIV -1 envelope antibodies can be found in the blood of HIV -1 patients and, consistently, the percentage of CD32 + CD4 T cells is increased in their blood. This CD32-mediated, antigen -independent cell communication mode transiently expands the receptor repertoire and functionality of immune cells. HIV -1 hijacks this mechanism by triggering the generation of trogocytosis-promoting autoantibodies to gain access to immune cells critical to its persistence.