Hong Zhang , Qun Wang , Sireesha Yalavarthi , Lukas Pekar , Steven Shamnoski , Liufang Hu , Laura Helming , Stefan Zielonka , Chunxiao Xu
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Concurrently, c-MET has been identified as a highly expressed tumor-associated antigen (TAA) in various solid and soft tumors.</p></div><div><h3>Methods</h3><p>In this study, we aimed to develop a bispecific antibody (BsAb) that targets both c-MET and CD137, optimizing the BsAb format and CD137 binder for efficient delivery of the CD137 agonist to the tumor microenvironment (TME). We employed a monovalent c-MET motif and a trimeric CD137 Variable Heavy domain of Heavy chain (VHH) for the BsAb design.</p></div><div><h3>Results</h3><p>Our results demonstrate that the c-MET x CD137 BsAb provides co-stimulation to T cells through cross-linking by c-MET-expressing tumor cells. Functional immune assays confirmed the enhanced efficacy and potency of the c-MET x CD137 BsAb, as indicated by activation of CD137 signaling, target cell killing, and cytokine release in various tumor cell lines. Furthermore, the combination of c-MET x CD137 BsAb with Pembrolizumab showed a dose-dependent enhancement of target-induced T cell cytokine release.</p></div><div><h3>Conclusion</h3><p>Overall, the c-MET x CD137 BsAb exhibits a promising developability profile as a tumor-targeted immune agonist by minimizing off-target effects while effectively delivering immune agonism. It has the potential to overcome resistance to anti-PD-(L)1 therapies.</p></div>","PeriodicalId":9507,"journal":{"name":"Cancer treatment and research communications","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2024-01-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.sciencedirect.com/science/article/pii/S2468294224000170/pdfft?md5=596c44fe3b0550f1678bc63b21ca8a9e&pid=1-s2.0-S2468294224000170-main.pdf","citationCount":"0","resultStr":"{\"title\":\"Development of a c-MET x CD137 bispecific antibody for targeted immune agonism in cancer immunotherapy\",\"authors\":\"Hong Zhang , Qun Wang , Sireesha Yalavarthi , Lukas Pekar , Steven Shamnoski , Liufang Hu , Laura Helming , Stefan Zielonka , Chunxiao Xu\",\"doi\":\"10.1016/j.ctarc.2024.100805\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><h3>Background</h3><p>Targeting the costimulatory receptor CD137 has shown promise as a therapeutic approach for cancer immunotherapy, resulting in anti-tumor efficacy demonstrated in clinical trials. 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引用次数: 0
摘要
背景靶向成本刺激受体 CD137 已显示出作为癌症免疫疗法治疗方法的前景,并在临床试验中取得了抗肿瘤疗效。然而,最初的 CD137 激动剂抗体乌利单抗(urelumab)和乌妥米单抗(utomilumab)分别因肝毒性或缺乏疗效而在临床试验中面临挑战。本研究旨在开发一种同时靶向 c-MET 和 CD137 的双特异性抗体(BsAb),优化 BsAb 格式和 CD137 粘合剂,以便将 CD137 激动剂高效递送至肿瘤微环境(TME)。结果我们的研究结果表明,c-MET x CD137 BsAb 可通过表达 c-MET 的肿瘤细胞的交联作用为 T 细胞提供协同刺激。功能性免疫测定证实了 c-MET x CD137 BsAb 的功效和效力得到了增强,这表现在 CD137 信号的激活、靶细胞的杀伤以及各种肿瘤细胞系中细胞因子的释放。此外,c-MET x CD137 BsAb 与 Pembrolizumab 联用可剂量依赖性地增强靶细胞诱导的 T 细胞细胞因子释放。它具有克服抗 PD-(L)1 疗法耐药性的潜力。
Development of a c-MET x CD137 bispecific antibody for targeted immune agonism in cancer immunotherapy
Background
Targeting the costimulatory receptor CD137 has shown promise as a therapeutic approach for cancer immunotherapy, resulting in anti-tumor efficacy demonstrated in clinical trials. However, the initial CD137 agonistic antibodies, urelumab and utomilumab, faced challenges in clinical trials due to the liver toxicity or lack of efficacy, respectively. Concurrently, c-MET has been identified as a highly expressed tumor-associated antigen (TAA) in various solid and soft tumors.
Methods
In this study, we aimed to develop a bispecific antibody (BsAb) that targets both c-MET and CD137, optimizing the BsAb format and CD137 binder for efficient delivery of the CD137 agonist to the tumor microenvironment (TME). We employed a monovalent c-MET motif and a trimeric CD137 Variable Heavy domain of Heavy chain (VHH) for the BsAb design.
Results
Our results demonstrate that the c-MET x CD137 BsAb provides co-stimulation to T cells through cross-linking by c-MET-expressing tumor cells. Functional immune assays confirmed the enhanced efficacy and potency of the c-MET x CD137 BsAb, as indicated by activation of CD137 signaling, target cell killing, and cytokine release in various tumor cell lines. Furthermore, the combination of c-MET x CD137 BsAb with Pembrolizumab showed a dose-dependent enhancement of target-induced T cell cytokine release.
Conclusion
Overall, the c-MET x CD137 BsAb exhibits a promising developability profile as a tumor-targeted immune agonist by minimizing off-target effects while effectively delivering immune agonism. It has the potential to overcome resistance to anti-PD-(L)1 therapies.
期刊介绍:
Cancer Treatment and Research Communications is an international peer-reviewed publication dedicated to providing comprehensive basic, translational, and clinical oncology research. The journal is devoted to articles on detection, diagnosis, prevention, policy, and treatment of cancer and provides a global forum for the nurturing and development of future generations of oncology scientists. Cancer Treatment and Research Communications publishes comprehensive reviews and original studies describing various aspects of basic through clinical research of all tumor types. The journal also accepts clinical studies in oncology, with an emphasis on prospective early phase clinical trials. Specific areas of interest include basic, translational, and clinical research and mechanistic approaches; cancer biology; molecular carcinogenesis; genetics and genomics; stem cell and developmental biology; immunology; molecular and cellular oncology; systems biology; drug sensitivity and resistance; gene and antisense therapy; pathology, markers, and prognostic indicators; chemoprevention strategies; multimodality therapy; cancer policy; and integration of various approaches. Our mission is to be the premier source of relevant information through promoting excellence in research and facilitating the timely translation of that science to health care and clinical practice.