Zhang Chang, Jiao Shasha, Zeng Dadi, Jiang Wen, Wang Rongjuan, Zheng Bin, Wang Min, Wang Shuang, Gui Xun
Mabwell (Shanghai) Bioscience Co. Ltd., 201210, Shanghai, China.
Beijing Kohnoor Science & Technology Co. Ltd., 102206, Beijing, China.
NPJ Precis Oncol. 2025 May 12;9(1):138. doi: 10.1038/s41698-025-00913-w.
Recent studies have uncovered evidences for pro-tumorigenic activities attributed to IL-11, prompting a renewed focus on therapeutic strategies targeting IL-11 signaling for anti-tumor treatment. Here, we introduce 9MW3811, a monoclonal antibody designed to neutralize IL-11 effectively. By disrupting the IL-11/IL-11Rα/gp130 complex, 9MW3811 inhibits JAK/STAT3 signaling, significantly reducing tumor growth in diverse mouse models. More importantly, 9MW3811 synergizes with anti-PD-1 therapy, even in PD-1 non-responsive models like CT26. Single-cell RNA-seq analysis reveals that 9MW3811 remodels the tumor microenvironment by enhancing CD8+ T cell infiltration and reversing T cell exhaustion via upregulated XCL1 and downregulated CCL7, boosting anti-tumor cytotoxicity. Furthermore, 9MW3811 counteracts PD-1-induced T cell exhaustion, with anti-PD-1 antibodies effectively mitigating PD-1 upregulation post-9MW3811 treatment. These compelling findings support ongoing clinical trials of 9MW3811, aiming to translate these preclinical insights into therapeutic benefits for cancer patients.
最近的研究发现了白细胞介素-11(IL-11)具有促肿瘤活性的证据,这促使人们重新关注针对IL-11信号通路的抗肿瘤治疗策略。在此,我们介绍9MW3811,一种旨在有效中和IL-11的单克隆抗体。通过破坏IL-11/IL-11Rα/gp130复合物,9MW3811抑制JAK/STAT3信号通路,显著降低多种小鼠模型中的肿瘤生长。更重要的是,9MW3811与抗PD-1疗法协同作用,即使在CT26等对PD-1无反应的模型中也是如此。单细胞RNA测序分析表明,9MW3811通过增强CD8 + T细胞浸润和上调XCL1及下调CCL7逆转T细胞耗竭,重塑肿瘤微环境,增强抗肿瘤细胞毒性。此外,9MW3811可抵消PD-1诱导的T细胞耗竭,抗PD-1抗体可有效减轻9MW3811治疗后PD-1的上调。这些令人信服的发现支持了9MW3811正在进行的临床试验,旨在将这些临床前的见解转化为癌症患者的治疗益处。
