CD146 bound to LCK promotes T cell receptor signaling and antitumor immune responses in mice

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Abstract

Initiation of T cell receptor (TCR) signaling involves the activation of the tyrosine kinase LCK; however, it is currently unclear how LCK is recruited and activated. Here, we have identified the membrane protein CD146 as an essential member of the TCR network for LCK activation. CD146 deficiency in T cells substantially impaired thymocyte development and peripheral activation, both of which depend on TCR signaling. CD146 was found to directly interact with the SH3 domain of coreceptor-free LCK via its cytoplasmic domain. Interestingly, we found CD146 to be present in both monomeric and dimeric forms in T cells, with the dimerized form increasing after TCR ligation. Increased dimerized CD146 recruited LCK and promoted LCK autophosphorylation. In tumor models, CD146 deficiency dramatically impaired the antitumor response of T cells. Together, our data reveal an LCK activation mechanism for TCR initiation. We also underscore a rational intervention based on CD146 for tumor immunotherapy.

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Duan, H., Jing, L., Jiang, X., Ma, Y., Wang, D., Xiang, J., … Yan, X. (2021). CD146 bound to LCK promotes T cell receptor signaling and antitumor immune responses in mice. Journal of Clinical Investigation, 131(21). https://doi.org/10.1172/JCI148568

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