IL23R-specific CAR Tregs for the treatment of Crohn’s disease

Yue Cui, Marion David, Laura Bouchareychas, Sandrine Rouquier, Satria Sajuthi, Marion Ayrault, Candice Navarin, Gregory Lara, Audrey Lafon, Gaëlle Saviane, Sonia Boulakirba, Alexandra Menardi, Alexandra Demory, Jihane Frikeche, Stephanie de la Forest Divonne Beghelli, Hsiaomei Heidi Lu, Celine Dumont, Tobias Abel, David Fenard, Maurus de la Rosa, Julie Gertner-Dardenne
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Abstract

Background and Aims Regulatory T cells (Tregs) are key regulators in maintaining tissue homeostasis. Disrupted immune homeostasis is associated with Crohn’s disease (CD) pathogenesis. Thus, Treg therapy represents a promising long-acting treatment to restore immune balance in the diseased intestine. CAR (Chimeric Antigen Receptor) T-cell therapy has revolutionized cancer treatment. This innovative approach also provides the opportunity to improve therapy for CD. By targeting a disease-relevant protein, Interleukin-23 receptor (IL23R), we engineered Tregs expressing IL23R-CAR for treating active CD. Methods Intestinal IL23R expression from active CD was verified by immunohistochemical analysis. Phenotypic and functional characteristics of IL23R-CAR Tregs were assessed using in vitro assays and their migration capacity was monitored in a xenograft tumor model. Transcriptomic and proteomic analyses were performed to associate molecular profiles with IL23R-CAR Treg activation against colon biopsy-derived cells from active CD patients. Results Our study showed that IL23R-CAR displayed negligible tonic signalling and strong signal-to-noise ratio. IL23R-CAR Tregs maintained regulatory phenotype during in vitro expansion, even when chronically exposed to proinflammatory cytokines and target antigen. IL23R engagement on IL23R-CAR Tregs triggered CAR-specific activation and significantly enhanced their suppressive activity. Also, IL23R-CAR Tregs migrated to IL23R-expressing tissue in humanized mice. Finally, IL23R-CAR Tregs elicited a specific activation against colon biopsy-derived cells from active CD, suggesting an efficient CAR engagement in active CD. Molecular profiling of CD patient biopsies also revealed transcriptomic and proteomic patterns associated with IL23R-CAR activation. Conclusions Overall, our results demonstrate that IL23R-CAR Tregs represent a promising therapy for active CD.
用于治疗克罗恩病的 IL23R 特异性 CAR Tregs
背景和目的 调节性 T 细胞(Tregs)是维持组织稳态的关键调节因子。免疫平衡的破坏与克罗恩病(CD)的发病机制有关。因此,Treg疗法是恢复病变肠道免疫平衡的一种前景广阔的长效疗法。CAR(嵌合抗原受体)T细胞疗法为癌症治疗带来了革命性的变化。这种创新方法也为改善 CD 的治疗提供了机会。通过靶向疾病相关蛋白--白细胞介素-23受体(IL23R),我们设计了表达IL23R-CAR的Tregs,用于治疗活动性CD。方法 通过免疫组化分析验证了活动性 CD 肠道 IL23R 的表达。通过体外实验评估了IL23R-CAR Tregs的表型和功能特征,并在异种移植肿瘤模型中监测了它们的迁移能力。针对活动性 CD 患者的结肠活检细胞,进行了转录组学和蛋白质组学分析,以将分子特征与 IL23R-CAR Treg 激活联系起来。结果 我们的研究表明,IL23R-CAR 的强直性信号可忽略不计,信噪比很高。即使长期暴露于促炎细胞因子和靶抗原,IL23R-CAR Tregs 在体外扩增过程中仍能保持调节表型。IL23R-CAR Tregs 上的 IL23R 可触发 CAR 特异性活化,并显著增强其抑制活性。此外,IL23R-CAR Tregs 还能迁移到人源化小鼠的 IL23R 表达组织中。最后,IL23R-CAR Tregs 对活动性 CD 的结肠活检衍生细胞产生了特异性激活,这表明 CAR 能有效参与活动性 CD。CD 患者活检组织的分子剖析也揭示了与 IL23R-CAR 激活相关的转录组和蛋白质组模式。结论 总体而言,我们的研究结果表明,IL23R-CAR Tregs 是一种治疗活动性 CD 的有前途的疗法。
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