Broadly reactive anti-VHH antibodies for characterizing, blocking, or activating nanobody-based CAR-T cells Article Swipe

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Blocking (statistics) Antibody Blocking antibody Chemistry Cell biology Computer science Biology Immunology Computer network

Scott McComb , Bianca Dupont , Alex Shepherd , Bigitha Bennychen , Anne Marcil , Laura Tamblyn , Shalini Raphael , Joey Sheff , Greg Hussack , Anna N. Moraitis , Cunle Wu , Annie Aubry , Christine Gadoury , Julie Lippens , Martine Pagé , Annie Fortin , Simon Joubert , Linda Lamoureux , Marie Parat , Pierre Plante , Félix Malenfant , Mauro Acchione , Petra Pohankova , Joe Schrag , Andrea Acel , Mathieu Coutu , Emma Smith , M. El Bakkouri , Jennifer J. Hill , Tammy‐Lynn Tremblay , Aziza Manceur , Sharlene Faulkes , John K. Webb , Ahmed Zafer , Qin Zhu , Tina Nguyen , Robert A. Pon , Risini D. Weeratna , Mehdi Arbabi‐Ghahroudi ·

YOU? · · 2025 · Open Access · · DOI: https://doi.org/10.1093/abt/tbaf011 · OA: W4411732853

Background Production of chimeric antigen receptor T cell (CAR-T) therapies depends on antibody reagents to label, isolate, and expand T cell products. We sought to create antibody tools specific for the variable domain of heavy-chain only antibodies (VHHs), also known as nanobodies, used in some CARs. Methods We immunized a mouse with VHH and selected two murine monoclonal antibodies (mAbs) that bind to distinct epitopes in conserved framework regions of llama-derived VHHs, and not to human VH domains. Anti-VHH mAbs were characterized by enzyme-linked immunosorbent assay, surface plasmon resonance, and hydrogen-deuterium exchange mass spectrometry; were then tested for cell/tissue labeling and for modulating cellular activity in VHH-CAR-T cells. Results We produced a high-quality dual-clonal anti-VHH antibody product and confirmed reactivity to over 98% of VHH proteins regardless of their antigenic specificity, with no reactivity to human or mouse IgG and reduced reactivity to conventional llama or alpaca IgG. Anti-VHH binding did not disrupt VHH/antigen interaction, and thus was appropriate for secondary labeling to assess cellular or tissue reactivity of VHH molecules. Despite not interfering with antigen binding, anti-VHH antibodies (Abs) potently blocked VHH-CAR-T activation and cytolytic killing of target cells. When immobilized, anti-VHH Abs induced strong activation and expansion of VHH CAR-T cells; with 730-fold mean expansion, &gt;94% CAR purity, and retained CD8/CD4 heterogeneity. Functionally, anti-VHH antibody-expanded CAR-T cells maintained strong antigen-specific activity without functional exhaustion. Conclusions Overall, these data identify useful anti-VHH mAbs that can be applied to better understand and manipulate VHH-based CAR-T cells or other VHH-based immunotherapies.