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Surface Proteomics Reveals CD72 as a Target for In Vitro–Evolved Nanobody-Based CAR-T Cells in KMT2A/MLL1-Rearranged B-ALL
- Nix, Matthew A;
- Mandal, Kamal;
- Geng, Huimin;
- Paranjape, Neha;
- Lin, Yu-Hsiu T;
- Rivera, Jose M;
- Marcoulis, Makeba;
- White, Kristie L;
- Whitman, Jeffrey D;
- Bapat, Sagar P;
- Parker, Kevin R;
- Ramirez, Jonathan;
- Deucher, Anne;
- Phojanokong, Paul;
- Steri, Veronica;
- Fattahi, Faranak;
- Hann, Byron C;
- Satpathy, Ansuman T;
- Manglik, Aashish;
- Stieglitz, Elliot;
- Wiita, Arun P
- et al.
Published Web Location
https://doi.org/10.1158/2159-8290.cd-20-0242Abstract
Alternative strategies are needed for patients with B-cell malignancy relapsing after CD19-targeted immunotherapy. Here, cell surface proteomics revealed CD72 as an optimal target for poor-prognosis KMT2A/MLL1-rearranged (MLLr) B-cell acute lymphoblastic leukemia (B-ALL), which we further found to be expressed in other B-cell malignancies. Using a recently described, fully in vitro system, we selected synthetic CD72-specific nanobodies, incorporated them into chimeric antigen receptors (CAR), and demonstrated robust activity against B-cell malignancy models, including CD19 loss. Taking advantage of the role of CD72 in inhibiting B-cell receptor signaling, we found that SHIP1 inhibition increased CD72 surface density. We establish that CD72-nanobody CAR-T cells are a promising therapy for MLLr B-ALL. SIGNIFICANCE: Patients with MLLr B-ALL have poor prognoses despite recent immunotherapy advances. Here, surface proteomics identifies CD72 as being enriched on MLLr B-ALL but also widely expressed across B-cell cancers. We show that a recently described, fully in vitro nanobody platform generates binders highly active in CAR-T cells and demonstrate its broad applicability for immunotherapy development.This article is highlighted in the In This Issue feature, p. 1861.
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