Cavβ1 regulates T cell expansion and apoptosis independently of voltage-gated Ca 2+ channel function

TCR stimulation triggers Ca signals that are critical for T cell function and immunity. Several pore-forming α and auxiliary β subunits of voltage-gated Ca channels (VGCC) were reported in T cells, but their mechanism of activation remains elusive and their contribution to Ca signaling in T cells is...

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Veröffentlicht in:Nature communications 2022-04, Vol.13 (1), p.2033
Hauptverfasser: Erdogmus, Serap, Concepcion, Axel R, Yamashita, Megumi, Sidhu, Ikjot, Tao, Anthony Y, Li, Wenyi, Rocha, Pedro P, Huang, Bonnie, Garippa, Ralph, Lee, Boram, Lee, Amy, Hell, Johannes W, Lewis, Richard S, Prakriya, Murali, Feske, Stefan
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Sprache:eng
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Zusammenfassung:TCR stimulation triggers Ca signals that are critical for T cell function and immunity. Several pore-forming α and auxiliary β subunits of voltage-gated Ca channels (VGCC) were reported in T cells, but their mechanism of activation remains elusive and their contribution to Ca signaling in T cells is controversial. We here identify Ca β1, encoded by Cacnb1, as a regulator of T cell function. Cacnb1 deletion enhances apoptosis and impairs the clonal expansion of T cells after lymphocytic choriomeningitis virus (LCMV) infection. By contrast, Cacnb1 is dispensable for T cell proliferation, cytokine production and Ca signaling. Using patch clamp electrophysiology and Ca recordings, we are unable to detect voltage-gated Ca currents or Ca influx in human and mouse T cells upon depolarization with or without prior TCR stimulation. mRNAs of several VGCC α1 subunits are detectable in human (Ca 3.3, Ca 3.2) and mouse (Ca 2.1) T cells, but they lack transcription of many 5' exons, likely resulting in N-terminally truncated and non-functional proteins. Our findings demonstrate that although Ca β1 regulates T cell function, these effects are independent of VGCC channel activity.
ISSN:2041-1723