Dysfunctional BTN3A together with deregulated immune checkpoints and type I/II IFN dictate defective interplay between pDCs and γδ T cells in melanoma patients, which impacts clinical outcomes.
Pauline GirardEleonora Sosa CuevasBenedicte PonsardStephane MouretHugo GilEdwige ColFlorence De FraipontNathalie SturmJulie CharlesOlivier ManchesLaurence ChaperotCaroline AspordPublished in: Clinical & translational immunology (2021)
Our study uncovered that melanoma hijacked the bidirectional interplay between pDCs and γδ T cells to escape from immune control, and revealed BTN3A dysfunction. Such understanding will help harness and synergise the power of these potent immune cells to design new therapeutic approaches exploiting their antitumor potential while counteracting their skewing by tumors to improve patient outcomes.