Human immunocompetent Organ-on-Chip platforms allow safety profiling of tumor-targeted T-cell bispecific antibodies

具有人类免疫活性的芯片器官平台能够对靶向肿瘤的T细胞双特异性抗体进行安全性分析

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作者:S Jordan Kerns # ,Chaitra Belgur # ,Debora Petropolis ,Marianne Kanellias ,Riccardo Barrile ,Johannes Sam ,Tina Weinzierl ,Tanja Fauti ,Anne Freimoser-Grundschober ,Jan Eckmann ,Carina Hage ,Martina Geiger ,Patrick Ray Ng ,William Tien-Street ,Dimitris V Manatakis ,Virginie Micallef ,Regine Gerard ,Michael Bscheider ,Ekaterina Breous-Nystrom ,Anneliese Schneider ,Anna Maria Giusti ,Cristina Bertinetti-Lapatki ,Heather Shannon Grant ,Adrian B Roth ,Geraldine A Hamilton ,Thomas Singer ,Katia Karalis ,Annie Moisan ,Peter Bruenker ,Christian Klein ,Marina Bacac ,Nikolce Gjorevski # ,Lauriane Cabon #

Abstract

Traditional drug safety assessment often fails to predict complications in humans, especially when the drug targets the immune system. Here, we show the unprecedented capability of two human Organs-on-Chips to evaluate the safety profile of T-cell bispecific antibodies (TCBs) targeting tumor antigens. Although promising for cancer immunotherapy, TCBs are associated with an on-target, off-tumor risk due to low levels of expression of tumor antigens in healthy tissues. We leveraged in vivo target expression and toxicity data of TCBs targeting folate receptor 1 (FOLR1) or carcinoembryonic antigen (CEA) to design and validate human immunocompetent Organs-on-Chips safety platforms. We discovered that the Lung-Chip and Intestine-Chip could reproduce and predict target-dependent TCB safety liabilities, based on sensitivity to key determinants thereof, such as target expression and antibody affinity. These novel tools broaden the research options available for mechanistic understandings of engineered therapeutic antibodies and assessing safety in tissues susceptible to adverse events.

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