CD5 expression by dendritic cells directs T cell immunity and sustains immunotherapy responses.

Alina Ulezko Antonova ,Stephen T. Ferris ,Nicholas Borcherding ,Daniel Korenfeld ,Yun Zhao ,Judah Gray ,Matthew M. Gubin ,Kairav Shah ,Thomas Tung ,Rasmus O. Bak ,Charles R. Schutt ,Robert L. Modlin ,Trine I. Jensen ,Cecilia S. Lindestam Arlehamn ,Feiyang Ma ,Robert D. Schreiber ,Jingqin Luo ,Laurent Gorvel ,Alessandro Sette ,Paul M. Allen ,David L. Donermeyer ,J. Michael White ,Sabrina Dinkel ,Ryan C. Fields ,Vince Garin ,Mingyu He ,Himanshi Bhatia ,Courtney A. Iberg ,Kate Roussak ,Matteo Pellegrini ,Eynav Klechevsky

doi:10.1126/science.abg2752

Abstract

The induction of proinflammatory T cells by dendritic cell (DC) subtypes is critical for antitumor responses and effective immune checkpoint blockade (ICB) therapy. Here, we show that human CD1c+CD5+ DCs are reduced in melanoma-affected lymph nodes, with CD5 expression on DCs correlating with patient survival. Activating CD5 on DCs enhanced T cell priming and improved survival after ICB therapy. CD5+ DC numbers increased during ICB therapy, and low interleukin-6 (IL-6) concentrations promoted their de novo differentiation. Mechanistically, CD5 expression by DCs was required to generate optimally protective CD5hi T helper and CD8+ T cells; further, deletion of CD5 from T cells dampened tumor elimination in response to ICB therapy in vivo. Thus, CD5+ DCs are an essential component of optimal ICB therapy.

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