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  • Compromised antigen binding and signaling interfere with bispecific CD19 and CD79a chimeric antigen receptor function.

Compromised antigen binding and signaling interfere with bispecific CD19 and CD79a chimeric antigen receptor function.

Blood advances (2022-12-06)
Isabel Leung, Megan L Templeton, Yun Lo, Anusha Rajan, Sylvia M Stull, Sarah M Garrison, Alexander I Salter, Kimberly S Smythe, Colin E Correnti, Shivani Srivastava, Cecilia C S Yeung, Stanley R Riddell
ABSTRACT

Therapy with CD19-directed chimeric antigen receptor (CAR) T cells has transformed the treatment of advanced B-cell malignancies. However, loss of or low antigen expression can enable tumor escape and limit the duration of responses achieved with CAR T-cell therapy. Engineering bispecific CAR T cells that target 2 tumor antigens could overcome antigen-negative escape. We found that CD79a and b, which are heterodimeric components of the B-cell receptor, were expressed on 84.3% of lymphoma cases using immunohistochemistry, and 87.3% of CD79ab-positive tumors also coexpressed CD19. We generated 3 bispecific permutations: tandem, bicistronic, and pooled products of CD79a-CD19 or CD79b-CD19 CAR T cells and showed that bispecific CAR T cells prevented the outgrowth of antigen-negative cells in a CD19-loss lymphoma xenograft model. However, tandem and bicistronic CAR T cells were less effective than monospecific CD19 or CD79a CAR T cells for the treatment of tumors that only expressed CD19 or CD79, respectively. When compared with monospecific CAR T cells, T cells expressing a tandem CAR exhibited reduced binding of each target antigen, and T cells expressing a bicistronic CAR vector exhibited reduced phosphorylation of downstream CAR signaling molecules. Our study showed that despite added specificity, tandem and bicistronic CAR T cells exhibit different defects that impair recognition of tumor cells expressing a single antigen. Our data provide support for targeting multiple B-cell antigens to improve efficacy and identify areas for improvement in bispecific receptor designs.

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Sigma-Aldrich
Anti-Cyclin D1 antibody, Rabbit monoclonal, clone SP4, recombinant, expressed in proprietary host, tissue culture supernatant