Selective elimination of immunosuppressive T cells in patients with multiple myeloma

Author:

Awwad Mohamed H. S.,Mahmoud Abdelrahman,Bruns Heiko,Echchannaoui Hakim,Kriegsmann Katharina,Lutz Raphael,Raab Marc S.,Bertsch Uta,Munder Markus,Jauch Anna,Weisel Katja,Maier Bettina,Weinhold Niels,Salwender Hans Jürgen,Eckstein Volker,Hänel Mathias,Fenk Roland,Dürig Jan,Brors BenediktORCID,Benner Axel,Müller-Tidow CarstenORCID,Goldschmidt HartmutORCID,Hundemer MichaelORCID

Abstract

AbstractElimination of suppressive T cells may enable and enhance cancer immunotherapy. Here, we demonstrate that the cell membrane protein SLAMF7 was highly expressed on immunosuppressive CD8+CD28-CD57+ Tregs in multiple myeloma (MM). SLAMF7 expression associated with T cell exhaustion surface markers and exhaustion-related transcription factor signatures. T cells from patients with a high frequency of SLAMF7+CD8+ T cells exhibited decreased immunoreactivity towards the MART-1aa26–35*A27L antigen. A monoclonal anti-SLAMF7 antibody (elotuzumab) specifically depleted SLAMF7+CD8+ T cells in vitro and in vivo via macrophage-mediated antibody-dependent cellular phagocytosis (ADCP). Anti-SLAMF7 treatment of MM patients depleted suppressive T cells in peripheral blood. These data highlight SLAMF7 as a marker for suppressive CD8+ Treg and suggest that anti-SLAMF7 antibodies can be used to boost anti-tumoral immune responses in cancer patients.

Funder

Bristol-Myers Squibb

Celgene

Publisher

Springer Science and Business Media LLC

Subject

Oncology,Cancer Research,Hematology

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