Phosphoantigeninduced Insideout Stabilization Of Butyrophilin Receptor Complexes Drives Dimerizationdependent γδ Tcr Activation Yuwei Zhu Wenbo Gao Jianlin Zheng Ye Bai Xinyu Tian Tengjin Huang Zebin Lu De Dong Anqi Zhang Changyou Guo Zhiwei Huang by Yuwei Zhu & Wenbo Gao & Jianlin Zheng & Ye Bai & Xinyu Tian & Tengjin Huang & Zebin Lu & De Dong & Anqi Zhang & Changyou Guo & Zhiwei Huang 101016/JIMMUNI202504012 instant download after payment.

SUMMARYPhosphoantigens (pAgs), produced by infected or cancer cells, trigger the assembly of a membrane receptorcomplex comprising butyrophilin (BTN) members BTN3A1 and BTN2A1, leading to the activation of γδ T cells.BTN3A2 or BTN3A3 forms heteromers with BTN3A1, exhibiting higher γδ T cell receptor (TCR)-stimulatingactivity than BTN3A1 homomers. Cryoelectron microscopy (cryo-EM) structure reveals a pAg-inducedBTN2A1-BTN3A1 heterotetramer with a 2:2 stoichiometry, stabilized by interactions between the intracellularB30.2 domains and the extracellular immunoglobulin V (IgV) domains. BTN3A2 or BTN3A3 heterodimerizeswith BTN3A1, forming a pAg-induced tetrameric complex with BTN2A1. However, BTN3A1 heterodimersare more stable than BTN3A1 homodimers in this interaction. Cryo-EM reveals that BTN2A1-BTN3A1-BTN3A2 binds two γδ TCR ectodomains, with one being sandwiched between the IgV domains of BTN2A1and BTN3A2, while the other interacts with the free BTN2A1 IgV in the complex, as evidenced by functionaldata. Together, our findings uncover the mechanism of ligand-induced inside-out stabilization of BTN receptor complexes for dimeric activation of γδ TCR.