PO.IM02.07 · 免疫学

HIS models lacking FcgammaR provide increased predictability and facilitate study design for evaluation of immuno-oncology therapeutics

海报缩略图:HIS models lacking FcgammaR provide increased predictability and facilitate study design for evaluation of immuno-oncology therapeutics
编号 6978 展板 6 时间 4/22 09:00–12:00 区域 Section 8 主讲 Monika Buczek, BS;M Phil;PhD
分会场 Novel Models of Immunotherapy Response
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作者与单位

Monika Buczek, Philip Dube, Nicholas Smith, Janell Richardson, Louise Baskin, Esther Andino, Debra Freer, Kathleen Bott

Taconic Biosciences, Inc., Rensselaer, NY

摘要 Abstract

Humanized immune system (HIS) mouse platforms that support durable human NK and T cell function are essential for evaluating CAR-NK and CAR-T therapies. Residual murine Fc gamma receptors (FcgammaRs) can confound interpretation of IgG-based therapeutics and engineered cell products. We compared hIL-15 NOG and FcgammaR-null FcResolv™ hIL-15 NOG mice engrafted with human NK cells and observed equivalent ≥12-week persistence and stable CD56⁺CD16⁺ profiles, enabling extended engineered-cell studies. In CD34⁺ HIS tumor models, anti-PD1 efficacy and pharmacodynamics were accurately detected only in FcResolv™ mice. FcgammaR-null HIS platforms improve predictive assessment of CAR-NK/CAR-T efficacy, trafficking, and off-target responses.
利益披露 Disclosure
M. Buczek, None.. P. Dube, None.. N. Smith, None.. L. Baskin, None.. E. Andino, None.. D. Freer, None.. K. Bott, None.

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