Identification of distinct cytotoxic granules as the origin of supramolecular attack particles in T lymphocytes

Cytotoxic T lymphocytes (CTL) kill malignant and infected cells through the directed release of cytotoxic proteins into the immunological synapse (IS). The cytotoxic protein granzyme B (GzmB) is released in its soluble form or in supramolecular attack particles (SMAP). We utilize synaptobrevin2-mRFP...

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Veröffentlicht in:Nature communications 2022-02, Vol.13 (1), p.1029-1029, Article 1029
Hauptverfasser: Chang, Hsin-Fang, Schirra, Claudia, Ninov, Momchil, Hahn, Ulrike, Ravichandran, Keerthana, Krause, Elmar, Becherer, Ute, Bálint, Štefan, Harkiolaki, Maria, Urlaub, Henning, Valitutti, Salvatore, Baldari, Cosima T., Dustin, Michael L., Jahn, Reinhard, Rettig, Jens
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Sprache:eng
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Zusammenfassung:Cytotoxic T lymphocytes (CTL) kill malignant and infected cells through the directed release of cytotoxic proteins into the immunological synapse (IS). The cytotoxic protein granzyme B (GzmB) is released in its soluble form or in supramolecular attack particles (SMAP). We utilize synaptobrevin2-mRFP knock-in mice to isolate fusogenic cytotoxic granules in an unbiased manner and visualize them alone or in degranulating CTLs. We identified two classes of fusion-competent granules, single core granules (SCG) and multi core granules (MCG), with different diameter, morphology and protein composition. Functional analyses demonstrate that both classes of granules fuse with the plasma membrane at the IS. SCG fusion releases soluble GzmB. MCGs can be labelled with the SMAP marker thrombospondin-1 and their fusion releases intact SMAPs. We propose that CTLs use SCG fusion to fill the synaptic cleft with active cytotoxic proteins instantly and parallel MCG fusion to deliver latent SMAPs for delayed killing of refractory targets. Cytotoxic T cells have specialised granules that are important for mediating their killing function. Here the authors characterise two types of cytotoxic granules and indicate different functions and temporal release of mediators at the immunological synapse.
ISSN:2041-1723
2041-1723
DOI:10.1038/s41467-022-28596-y