1. Tuning of in vivo cognate B-T cell interactions by Intersectin 2 is required for effective anti-viral B cell immunity
- Author
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Francesca Gasparrini, Marianne Burbage, Shweta Aggarwal, Andreas Bruckbauer, Michael Way, Mauro Gaya, Usha Nair, Johan Arnold, and Facundo D. Batista
- Subjects
Life Sciences & Biomedicine - Other Topics ,0301 basic medicine ,Mouse ,T-Lymphocytes ,CDC42 ,Mice ,0302 clinical medicine ,Immunology and Inflammation ,GERMINAL CENTER ,Biology (General) ,GENE-PRODUCT ,antibody responses ,TRANSGENIC MICE ,B-Lymphocytes ,General Neuroscience ,Wiskott-Aldrich syndrome ,Signal transducing adaptor protein ,General Medicine ,Orthomyxoviridae ,3. Good health ,Cell biology ,medicine.anatomical_structure ,Influenza Vaccines ,Medicine ,B-T interactions ,Life Sciences & Biomedicine ,SAP ,Research Article ,QH301-705.5 ,T cell ,Science ,ANTIGEN ,macromolecular substances ,Biology ,General Biochemistry, Genetics and Molecular Biology ,03 medical and health sciences ,Immune system ,Antigen ,Orthomyxoviridae Infections ,medicine ,Cell Adhesion ,Animals ,HUMORAL IMMUNITY ,N-WASP ,LYMPH-NODE ,ACTIN POLYMERIZATION ,B cell ,Cell Proliferation ,B cells ,Science & Technology ,General Immunology and Microbiology ,Germinal center ,Survival Analysis ,SLAM family receptors ,Adaptor Proteins, Vesicular Transport ,030104 developmental biology ,Intersectin 2 ,030215 immunology - Abstract
Wiskott-Aldrich syndrome (WAS) is an immune pathology associated with mutations in WAS protein (WASp) or in WASp interacting protein (WIP). Together with the small GTPase Cdc42 and other effectors, these proteins participate in the remodelling of the actin network downstream of BCR engagement. Here we show that mice lacking the adaptor protein ITSN2, a G-nucleotide exchange factor (GEF) for Cdc42 that also interacts with WASp and WIP, exhibited increased mortality during primary infection, incomplete protection after Flu vaccination, reduced germinal centre formation and impaired antibody responses to vaccination. These defects were found, at least in part, to be intrinsic to the B cell compartment. In vivo, ITSN2 deficient B cells show a reduction in the expression of SLAM, CD84 or ICOSL that correlates with a diminished ability to form long term conjugates with T cells, to proliferate in vivo, and to differentiate into germinal centre cells. In conclusion, our study not only revealed a key role for ITSN2 as an important regulator of adaptive immune-response during vaccination and viral infection but it is also likely to contribute to a better understanding of human immune pathologies.
- Published
- 2018