Signal transduction through Vav-2 participates in humoral immune responses and B cell maturation

GM Doody, SE Bell, E Vigorito, E Clayton… - Nature …, 2001 - nature.com
GM Doody, SE Bell, E Vigorito, E Clayton, S McAdam, R Tooze, C Fernandez, IJ Lee…
Nature immunology, 2001nature.com
B and T lymphocytes develop normally in mice lacking the guanine nucleotide exchange
factor Vav-2. However, the immune responses to type II thymus-independent antigen as well
as the primary response to thymus-dependent (TD) antigen are defective. Vav-2–deficient
mice are also defective in their ability to switch immunoglobulin class, form germinal centers
and generate secondary immune responses to TD antigens. Mice lacking both Vav-1 and
Vav-2 contain reduced numbers of B lymphocytes and display a maturational block in the …
Abstract
B and T lymphocytes develop normally in mice lacking the guanine nucleotide exchange factor Vav-2. However, the immune responses to type II thymus-independent antigen as well as the primary response to thymus-dependent (TD) antigen are defective. Vav-2–deficient mice are also defective in their ability to switch immunoglobulin class, form germinal centers and generate secondary immune responses to TD antigens. Mice lacking both Vav-1 and Vav-2 contain reduced numbers of B lymphocytes and display a maturational block in the development of mature B cells. B cells from Vav-1−/− Vav-2−/− mice respond poorly to antigen receptor triggering, both in terms of proliferation and calcium release. These studies show the importance of Vav-2 in humoral immune responses and B cell maturation.
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