INHBA promotes tumor growth and induces resistance to PD-L1 blockade by suppressing IFN-γ signaling.

IF 6.9 1区 医学 Q1 CHEMISTRY, MULTIDISCIPLINARY Acta Pharmacologica Sinica Pub Date : 2024-09-02 DOI:10.1038/s41401-024-01381-x
Fang-Lin Li, Long-Hua Gu, Yong-Liang Tong, Run-Qiu Chen, Shi-Yi Chen, Xiao-Lu Yu, Nan Liu, Jiang-Ling Lu, Yuan Si, Jian-Hua Sun, Jing Chen, Yi-Ru Long, Li-Kun Gong
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Abstract

Inhibin beta A (INHBA) and its homodimer activin A have pleiotropic effects on modulation of immune responses and tumor progression, but it remains uncertain whether tumors may release activin A to regulate anti-tumor immunity. In this study we investigated the effects and mechanisms of tumor intrinsic INHBA on carcinogenesis, tumor immunity and PD-L1 blockade. Bioinformatic analysis on the TCGA database revealed that INHBA expression levels were elevated in 33 cancer types, including breast cancer (BRCA) and colon adenocarcinoma (COAD). In addition, survival analysis also corroborated that INHBA expression was negatively correlated with the prognosis of many types of cancer patients. We demonstrated that gain or loss function of Inhba did not alter in vitro growth of colorectal cancer CT26 cells, but had striking impact on mouse tumor models including CT26, MC38, B16 and 4T1 models. By using the TIMER 2.0 tool, we figured out that in most cancer types, Inhba expression in tumors was inversely associated with the infiltration of CD4+ T and CD8+ T cells. In CT26 tumor-bearing mice, overexpression of tumor INHBA eliminated the anti-tumor effect of the PD-L1 antibody atezolizumab, whereas INHBA deficiency enhanced the efficacy of atezolizumab. We revealed that tumor INHBA significantly downregulated the interferon-γ (IFN-γ) signaling pathway. Tumor INHBA overexpression led to lower expression of PD-L1 induced by IFN-γ, resulting in poor responsiveness to anti-PD-L1 treatment. On the other hand, decreased secretion of IFN-γ-stimulated chemokines, including C-X-C motif chemokine 9 (CXCL9) and 10 (CXCL10), impaired the infiltration of effector T cells into the tumor microenvironment (TME). Furthermore, the activin A-specific antibody garetosmab improved anti-tumor immunity and its combination with the anti-PD-L1 antibody atezolizumab showed a superior therapeutic effect to monotherapy with garetosmab or atezolizumab. We demonstrate that INHBA and activin A are involved in anti-tumor immunity by inhibiting the IFN-γ signaling pathway, which can be considered as potential targets to improve the responsive rate of PD-1/PD-L1 blockade.

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INHBA 通过抑制 IFN-γ 信号传导,促进肿瘤生长并诱导对 PD-L1 阻断剂的抗性。
抑制素βA(INHBA)及其同源二聚体激活素A对免疫反应和肿瘤进展具有多向效应,但肿瘤是否会释放激活素A来调节抗肿瘤免疫仍不确定。在本研究中,我们研究了肿瘤内在 INHBA 对癌变、肿瘤免疫和 PD-L1 阻断的影响和机制。TCGA数据库的生物信息学分析表明,INHBA在33种癌症类型中表达水平升高,包括乳腺癌(BRCA)和结肠腺癌(COAD)。此外,生存分析也证实,INHBA 的表达与多种癌症患者的预后呈负相关。我们证实,Inhba 的功能增益或缺失不会改变结直肠癌 CT26 细胞的体外生长,但会对 CT26、MC38、B16 和 4T1 等小鼠肿瘤模型产生显著影响。通过使用 TIMER 2.0 工具,我们发现在大多数癌症类型中,Inhba 在肿瘤中的表达与 CD4+ T 和 CD8+ T 细胞的浸润成反比。在CT26肿瘤小鼠中,肿瘤INHBA的过表达消除了PD-L1抗体atezolizumab的抗肿瘤作用,而INHBA的缺乏则增强了atezolizumab的疗效。我们发现,肿瘤INHBA能显著下调干扰素-γ(IFN-γ)信号通路。肿瘤INHBA的过度表达导致IFN-γ诱导的PD-L1表达降低,从而导致对抗PD-L1治疗的反应性降低。另一方面,IFN-γ 刺激的趋化因子(包括 C-X-C motif 趋化因子 9 (CXCL9) 和 10 (CXCL10))分泌减少,影响了效应 T 细胞对肿瘤微环境(TME)的浸润。此外,活化素A特异性抗体加瑞妥单抗(garetosmab)提高了抗肿瘤免疫力,它与抗PD-L1抗体阿特珠单抗(atezolizumab)的联合治疗效果优于加瑞妥单抗或阿特珠单抗的单药治疗。我们证明,INHBA和激活素A通过抑制IFN-γ信号通路参与抗肿瘤免疫,可被视为提高PD-1/PD-L1阻断反应率的潜在靶点。
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
Acta Pharmacologica Sinica
Acta Pharmacologica Sinica 医学-化学综合
CiteScore
15.10
自引率
2.40%
发文量
4365
审稿时长
2 months
期刊介绍: APS (Acta Pharmacologica Sinica) welcomes submissions from diverse areas of pharmacology and the life sciences. While we encourage contributions across a broad spectrum, topics of particular interest include, but are not limited to: anticancer pharmacology, cardiovascular and pulmonary pharmacology, clinical pharmacology, drug discovery, gastrointestinal and hepatic pharmacology, genitourinary, renal, and endocrine pharmacology, immunopharmacology and inflammation, molecular and cellular pharmacology, neuropharmacology, pharmaceutics, and pharmacokinetics. Join us in sharing your research and insights in pharmacology and the life sciences.
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