Both APRIL and antibody-fragment-based CAR T cells for myeloma induce BCMA downmodulation by trogocytosis and internalization

Nicolas Camviel; Benita Wolf; Giancarlo Croce; David Gfeller; Vincent Zoete; Caroline Arber

doi:10.1136/jitc-2022-005091

Both APRIL and antibody-fragment-based CAR T cells for myeloma induce BCMA downmodulation by trogocytosis and internalization

J Immunother Cancer. 2022 Nov;10(11):e005091. doi: 10.1136/jitc-2022-005091.

Authors

Nicolas Camviel^{1

2}, Benita Wolf^{1

2}, Giancarlo Croce^{1

2

3}, David Gfeller^{1

2

3}, Vincent Zoete^{1

2

3}, Caroline Arber^{4

2}

Affiliations

¹ Department of Oncology UNIL CHUV, Lausanne University Hospital (CHUV) and University of Lausanne (UNIL), Lausanne, Switzerland.
² Ludwig Institute for Cancer Research Lausanne Branch, Lausanne, Switzerland.
³ Swiss Institute of Bioinformatics (SIB), Lausanne, Switzerland.
⁴ Department of Oncology UNIL CHUV, Lausanne University Hospital (CHUV) and University of Lausanne (UNIL), Lausanne, Switzerland caroline.arber@unil.ch.

Abstract

Background: Chimeric antigen receptor (CAR) T cell therapy targeting B cell maturation antigen (BCMA) on multiple myeloma (MM) produces fast but not long-lasting responses. Reasons for treatment failure are poorly understood. CARs simultaneously targeting two antigens may represent an alternative. Here, we (1) designed and characterized novel A proliferation inducing ligand (APRIL) based dual-antigen targeting CARs, and (2) investigated mechanisms of resistance to CAR T cells with three different BCMA-binding moieties (APRIL, single-chain-variable-fragment, heavy-chain-only).

Methods: Three new APRIL-CARs were designed and characterized. Human APRIL-CAR T cells were evaluated for their cytotoxic function in vitro and in vivo, for their polyfunctionality, immune synapse formation, memory, exhaustion phenotype and tonic signaling activity. To investigate resistance mechanisms, we analyzed BCMA levels and cellular localization and quantified CAR T cell-target cell interactions by live microscopy. Impact on pathway activation and tumor cell proliferation was assessed in vitro and in vivo.

Results: APRIL-CAR T cells in a trimeric ligand binding conformation conferred fast but not sustained antitumor responses in vivo in mouse xenograft models. In vitro trimer-BBζ CAR T cells were more polyfunctional and formed stronger immune synapses than monomer-BBζ CAR T cells. After CAR T cell-myeloma cell contact, BCMA was rapidly downmodulated on target cells with all evaluated binding moieties. CAR T cells acquired BCMA by trogocytosis, and BCMA on MM cells was rapidly internalized. Since BCMA can be re-expressed during progression and persisting CAR T cells may not protect patients from relapse, we investigated whether non-functional CAR T cells play a role in tumor progression. While CAR T cell-MM cell interactions activated BCMA pathway, we did not find enhanced tumor growth in vitro or in vivo.

Conclusion: Antitumor responses with APRIL-CAR T cells were fast but not sustained. Rapid BCMA downmodulation occurred independently of whether an APRIL or antibody-based binding moiety was used. BCMA internalization mostly contributed to this effect, but trogocytosis by CAR T cells was also observed. Our study sheds light on the mechanisms underlying CAR T cell failure in MM when targeting BCMA and can inform the development of improved treatment strategies.

Keywords: T-lymphocytes; cell engineering; hematologic neoplasms; immunotherapy; receptors, chimeric antigen.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
B-Cell Maturation Antigen / genetics
B-Cell Maturation Antigen / metabolism
Humans
Ligands
Mice
Multiple Myeloma*
Neoplasm Recurrence, Local / metabolism
Receptors, Chimeric Antigen*
Single-Chain Antibodies*
T-Lymphocytes
Trogocytosis

Substances

B-Cell Maturation Antigen
Receptors, Chimeric Antigen
TNFSF13 protein, human
Ligands
Single-Chain Antibodies