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特异性阻断αvβ8介导的转化生长因子-β信号通路,通过调节巨噬细胞极化来逆转免疫抑制。

Specifically blocking αvβ8-mediated TGF-β signaling to reverse immunosuppression by modulating macrophage polarization.

作者信息

Guo Cuicui, Sun Hui, Du Yulei, Dai Xiaodong, Pang Yu, Han Zhen, Xiong Xinhui, Li Shaowei, Zhang Junhua, Zheng Qingbing, Gui Xun

机构信息

Mabwell (Shanghai) Bioscience Co., Ltd, Shanghai, 201210, China.

State Key Laboratory of Vaccines for Infectious Diseases, National Institute of Diagnostics and Vaccine Development in Infectious Diseases, School of Public Health, Xiamen University, Xiamen, China.

出版信息

J Exp Clin Cancer Res. 2025 Jan 2;44(1):1. doi: 10.1186/s13046-024-03250-1.

Abstract

BACKGROUND

Targeting the TGF-β pathway in tumor therapy has proven challenging due to the highly context-dependent functions of TGF-β. Integrin αvβ8, a pivotal activator of TGF-β, has been implicated in TGF-β signaling within tumors, as demonstrated by the significant anti-tumor effects of anti-αvβ8 antibodies. Nevertheless, the expression profile of αvβ8 remains a subject of debate, and the precise mechanisms underlying the anti-tumor effects of anti-αvβ8 antibodies are not yet fully elucidated.

METHODS

We utilized single-cell RNA sequencing to assess αvβ8 expression across various human tumors. An anti-αvβ8 antibody was developed and characterized for its binding and blocking properties in vitro. Cryo-EM single-particle analysis was employed to study the detailed interaction between αvβ8 and the antibody Fab fragment. The anti-tumor efficacy of the antibody was evaluated in syngeneic mouse models with varying levels of αvβ8 expression, both as a monotherapy and in combination with PD-1 antibodies. Human PBMCs were isolated to investigate αvβ8 expression in myeloid cells, and macrophages were exposed to the antibody to study its impact on macrophage polarization. Pharmacokinetic studies of the αvβ8 antibody were conducted in cynomolgus monkeys.

RESULTS

Integrin αvβ8 is notably expressed in certain tumor types and tumor-infiltrating macrophages. The specific αvβ8 antibody 130H2 demonstrated high affinity, specificity, and blocking potency in vitro. Cryo-EM analysis further revealed that 130H2 interacts exclusively with the β8 subunit, without binding to the αv subunit. In vivo studies showed that this antibody significantly inhibited tumor growth and alleviated immunosuppression by promoting immune cell infiltration. Furthermore, combining the antibody with PD-1 inhibition produced a synergistic anti-tumor effect. In human PBMCs, monocytes exhibited high αvβ8 expression, and the antibody directly modulated macrophage polarization. Tumors with elevated αvβ8 expression were particularly responsive to 130H2 treatment. Additionally, favorable pharmacokinetic properties were observed in cynomolgus monkeys.

CONCLUSIONS

In summary, integrin αvβ8 is highly expressed in certain tumors and tumor-infiltrating macrophages. Targeting αvβ8 with a blocking antibody significantly inhibits tumor growth by modulating macrophage polarization and enhancing immune cell infiltration. Combining αvβ8 targeting with PD-1 treatment markedly increases the sensitivity of immune-excluded tumors. These results support further clinical evaluation of αvβ8 antibodies.

摘要

背景

由于转化生长因子-β(TGF-β)的功能高度依赖于环境,因此在肿瘤治疗中靶向TGF-β信号通路具有挑战性。整合素αvβ8是TGF-β的关键激活因子,已被证明参与肿瘤内的TGF-β信号传导,抗αvβ8抗体的显著抗肿瘤作用证明了这一点。然而,αvβ8的表达谱仍存在争议,抗αvβ8抗体抗肿瘤作用的精确机制尚未完全阐明。

方法

我们利用单细胞RNA测序来评估αvβ8在各种人类肿瘤中的表达。开发了一种抗αvβ8抗体,并对其体外结合和阻断特性进行了表征。采用冷冻电镜单颗粒分析来研究αvβ8与抗体Fab片段之间的详细相互作用。在具有不同αvβ8表达水平的同基因小鼠模型中评估了该抗体的抗肿瘤疗效,既作为单一疗法,也与PD-1抗体联合使用。分离人外周血单核细胞(PBMC)以研究髓系细胞中αvβ8的表达,并将巨噬细胞暴露于该抗体以研究其对巨噬细胞极化的影响。在食蟹猴中进行了αvβ8抗体的药代动力学研究。

结果

整合素αvβ8在某些肿瘤类型和肿瘤浸润巨噬细胞中显著表达。特异性αvβ8抗体130H2在体外表现出高亲和力、特异性和阻断效力。冷冻电镜分析进一步表明,130H2仅与β8亚基相互作用,不与αv亚基结合。体内研究表明,该抗体通过促进免疫细胞浸润显著抑制肿瘤生长并减轻免疫抑制。此外,将该抗体与PD-1抑制联合使用产生了协同抗肿瘤作用。在人PBMC中,单核细胞表现出高αvβ8表达,并且该抗体直接调节巨噬细胞极化。αvβ8表达升高的肿瘤对130H2治疗特别敏感。此外,在食蟹猴中观察到了良好的药代动力学特性。

结论

总之,整合素αvβ8在某些肿瘤和肿瘤浸润巨噬细胞中高度表达。用阻断抗体靶向αvβ8可通过调节巨噬细胞极化和增强免疫细胞浸润来显著抑制肿瘤生长。将αvβ8靶向与PD-1治疗相结合可显著提高免疫排除型肿瘤的敏感性。这些结果支持对αvβ8抗体进行进一步的临床评估。

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