Targeting TNFRSF25 by agonistic antibodies and multimeric TL1A proteins co-stimulated CD8⁺ T cells and inhibited tumor growth.

IF 10.3 1区医学 Q1 IMMUNOLOGY

Journal for Immunotherapy of Cancer Pub Date : 2024-08-13 DOI:10.1136/jitc-2024-008810

Xueyuan Lyu, Linlin Zhao, Sijia Chen, Yulu Li, Yajing Yang, Huisi Liu, Fang Yang, Wenhui Li, Jianhua Sui

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引用次数: 0

Abstract

Background: Tumor necrosis factor receptor superfamily 25 (TNFRSF25) is a T-cell co-stimulatory receptor. Expression of its ligand, TNF-like cytokine 1A (TL1A), on mouse tumor cells has been shown to promote tumor regression. This study aimed to develop TNFRSF25 agonists (both antibodies (Abs) and TL1A proteins) and to investigate their potential antitumor effects.

Methods: Anti-mouse TNFRSF25 (mTNFRSF25) Abs and multimeric TL1A proteins were generated as TNFRSF25 agonists. Their agonism was assessed in luciferase reporter and T-cell co-stimulation assays, and their antitumor effects were evaluated in syngeneic mouse tumor models. TNFRSF25 expression within the tumor microenvironment and the effects of an anti-mTNFRSF25 agonistic Ab on tumor-infiltrating T cells were evaluated by flow cytometry. Cell depletion assays were used to identify the immune cell types that contribute to the antitumor effect of the anti-mTNFRSF25 Ab. The Fc gamma receptor (FcγR) dependence of TNFRSF25 agonists was assessed in an in vivo T-cell expansion model and a mouse tumor model using Fc variants and FcγR-deficient mice.

Results: TNFRSF25 agonists exhibited antitumor effects in syngeneic mouse tumor models without causing observed side effects. We identified an anti-mTNFRSF25 agonistic Ab, 1A6-m1, which exhibited greater antitumor activity than a higher affinity anti-TNFRSF25 Ab which engages an overlapping epitope with 1A6-m1. 1A6-m1 activated CD8⁺ T cells and antigen-specific T cells, leading to tumor regression; it also induced long-term antitumor immune memory. Although activating TNFRSF25 by 1A6-m1 expanded splenic regulatory T (Treg) cells, it did not influence intratumoral Treg cells. Moreover, 1A6-m1's antitumor effects required the engagement of both inhibitory FcγRIIB and activating FcγRIII. Replacing 1A6-m1's CH1-hinge region with that of human IgG2 (h2) conferred enhanced antitumor effects. Finally, we also generated multimeric human and mouse TL1A fusion proteins as TNFRSF25 agonists, and they co-stimulated CD8⁺ T cells and reduced tumor growth, even in the absence of Fc-FcγR interactions.

Conclusion: Our data demonstrates the potential of activating TNFRSF25 by Abs and multimeric TL1A proteins for cancer immunotherapy and provides insights into their development astherapeutics.

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通过激动抗体和多聚 TL1A 蛋白靶向 TNFRSF25，可共同刺激 CD8+ T 细胞并抑制肿瘤生长。

背景：肿瘤坏死因子受体超家族 25（TNFRSF25）是一种 T 细胞共刺激受体。在小鼠肿瘤细胞上表达其配体 TNF 样细胞因子 1A（TL1A）已被证明可促进肿瘤消退。本研究旨在开发 TNFRSF25 激动剂（抗体（Abs）和 TL1A 蛋白），并研究其潜在的抗肿瘤作用：方法：制备了抗小鼠 TNFRSF25（mTNFRSF25）Abs 和多聚 TL1A 蛋白作为 TNFRSF25 激动剂。在荧光素酶报告和 T 细胞共刺激试验中评估了它们的激动作用，并在合成小鼠肿瘤模型中评估了它们的抗肿瘤效果。流式细胞术评估了肿瘤微环境中 TNFRSF25 的表达以及抗 mTNFRSF25 激动剂 Ab 对肿瘤浸润 T 细胞的影响。细胞耗竭试验被用来确定有助于抗mTNFRSF25抗体抗肿瘤作用的免疫细胞类型。在体内T细胞扩增模型和使用Fc变体和FcγR缺陷小鼠的小鼠肿瘤模型中评估了TNFRSF25激动剂对Fcγ受体（FcγR）的依赖性：结果：TNFRSF25激动剂在合成小鼠肿瘤模型中表现出抗肿瘤效果，且不会引起观察到的副作用。我们发现了一种抗 mTNFRSF25 激动剂抗体 1A6-m1，它比亲和力更高的抗 TNFRSF25 抗体具有更强的抗肿瘤活性，后者与 1A6-m1 的表位重叠。1A6-m1 能激活 CD8+ T 细胞和抗原特异性 T 细胞，导致肿瘤消退；它还能诱导长期抗肿瘤免疫记忆。虽然1A6-m1激活TNFRSF25能扩增脾脏调节性T（Treg）细胞，但并不影响瘤内Treg细胞。此外，1A6-m1的抗肿瘤作用需要抑制性FcγRIIB和激活性FcγRIII的参与。将 1A6-m1 的 CH1 铰链区替换为人 IgG2（h2）的 CH1 铰链区可增强抗肿瘤效果。最后，我们还生成了多聚人和小鼠 TL1A 融合蛋白作为 TNFRSF25 激动剂，即使在没有 Fc-FcγR 相互作用的情况下，它们也能共同刺激 CD8+ T 细胞并减少肿瘤生长：我们的数据证明了 Abs 和多聚 TL1A 蛋白激活 TNFRSF25 用于癌症免疫疗法的潜力，并为它们作为治疗药物的开发提供了启示。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal for Immunotherapy of Cancer Biochemistry, Genetics and Molecular Biology-Molecular Medicine

CiteScore

17.70

自引率

4.60%

发文量

522

审稿时长

18 weeks

期刊介绍： The Journal for ImmunoTherapy of Cancer (JITC) is a peer-reviewed publication that promotes scientific exchange and deepens knowledge in the constantly evolving fields of tumor immunology and cancer immunotherapy. With an open access format, JITC encourages widespread access to its findings. The journal covers a wide range of topics, spanning from basic science to translational and clinical research. Key areas of interest include tumor-host interactions, the intricate tumor microenvironment, animal models, the identification of predictive and prognostic immune biomarkers, groundbreaking pharmaceutical and cellular therapies, innovative vaccines, combination immune-based treatments, and the study of immune-related toxicity.