The pre-existing T cell landscape determines the response to bispecific T cell engagers in multiple myeloma patients

Mirco Friedrich(Broad Institute), Paola Neri(Ontario Institute for Cancer Research), Niklas Kehl(German Cancer Research Center), Julius Michel(German Cancer Research Center), Simon Steiger(German Cancer Research Center), Michael Kilian(German Cancer Research Center), Noémie Leblay, Ranjan Maity, Roman Sankowski(University Medical Center Freiburg), Holly Lee(Ontario Institute for Cancer Research), Elie Barakat, Sungwoo Ahn, Niels Weinhold(Heidelberg University), Karsten Rippe(German Cancer Research Center), Lukas Bunse(German Cancer Research Center), Michael Platten(German Cancer Research Center), Hartmut Goldschmidt(Heidelberg University), Carsten Müller‐Tidow(Heidelberg University), Marc‐Steffen Raab(German Cancer Research Center), Nizar J. Bahlis(Ontario Institute for Cancer Research)
Cancer Cell
March 9, 2023
Cited by 241Open Access
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Abstract

Bispecific T cell engagers (TCEs) have shown promise in the treatment of various cancers, but the immunological mechanism and molecular determinants of primary and acquired resistance to TCEs remain poorly understood. Here, we identify conserved behaviors of bone marrow-residing T cells in multiple myeloma patients undergoing BCMAxCD3 TCE therapy. We show that the immune repertoire reacts to TCE therapy with cell state-dependent clonal expansion and find evidence supporting the coupling of tumor recognition via major histocompatibility complex class I (MHC class I), exhaustion, and clinical response. We find the abundance of exhausted-like CD8+ T cell clones to be associated with clinical response failure, and we describe loss of target epitope and MHC class I as tumor-intrinsic adaptations to TCEs. These findings advance our understanding of the in vivo mechanism of TCE treatment in humans and provide the rationale for predictive immune-monitoring and conditioning of the immune repertoire to guide future immunotherapy in hematological malignancies.


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