Ginsenoside Rh2 in combination with IFNγ potentiated the anti-cancer effect by enhancing interferon signaling response in colorectal cancer cells.

IF 6.9 1区医学 Q1 CHEMISTRY, MULTIDISCIPLINARY

Acta Pharmacologica Sinica Pub Date : 2025-04-22 DOI:10.1038/s41401-025-01557-z

Mu-Yang Huang, Chun-Cao Xu, Qian Chen, Yan-Ming Zhang, Wen-Yu Lyu, Zi-Han Ye, Ting Li, Ming-Qing Huang, Jin-Jian Lu

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Abstract

Interferon gamma (IFNγ) can amplify immune cell-mediated anti-tumor immunity, as well as directly kill cancer cells. Ginsenoside Rh2 (Rh2), a bioactive compound in traditional Chinese medicine, exhibits anti-cancer effects such as inhibiting proliferation and metastasis. Our earlier research found that Rh2 combined with IFNγ enhanced CXCL10 secretion in cancer cells. Here, we explored whether Rh2 and IFNγ exerted more potent anti-cancer activity in vitro and in vivo, along with its mechanisms and clinical value. Our data showed that Rh2 in combination with IFNγ resulted in a remarkably increased cytotoxicity in colorectal cancer cells including HT29, LoVo and T84 cell lines. Consistently, intratumoral injection with Rh2 plus IFNγ further restricted the HT29 tumor growth in vivo, and importantly, it was demonstrated to be safe for mice. Meanwhile, the combo treatment activated the stimulator of interferon genes (STING) pathway in cancer cells, promoting the transcription of downstream type I interferon. RNA sequencing revealed a dramatically transcriptional alteration in cancer cells with combo treatment and indicated that Rh2 further augmented the activation of interferon signaling pathway, compared with the IFNγ alone. Inhibition of janus kinase (JAK) by ruxolitinib could significantly rescue the cell death-triggered by the combo treatment. Then, a gene set named Rh2+IFNγ signature genes (RISG) was defined, which contained top 20 significantly upregulated genes from the combo treatment. Patients who exhibited a favorable response to the immunotherapy had a higher expression of RISG in tumor compared with those who did not respond. And the high expression of RISG was correlated with better clinical outcome in patients with colorectal cancer (CRC) and skin cutaneous melanoma (SKCM). Herein, the combination of Rh2 with IFNγ served as a promising strategy for cancer treatment, and its-derived RISG gene set also exhibited potential value in predicting clinical outcome. Schematic diagram of the anti-cancer effect of Rh2 combined with IFNγ. The schematic diagram illustrated that ginsenoside Rh2 in combination with IFNγ robustly activated the interferon signals in cancer cells, ultimately leading a significant cell death of cancer cells. ISGs, interferon-stimulated genes. Created with BioRender.com.

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人参皂苷Rh2与IFNγ联合作用通过增强结直肠癌细胞的干扰素信号应答来增强其抗癌作用。

干扰素γ (IFNγ)可以增强免疫细胞介导的抗肿瘤免疫，也可以直接杀死癌细胞。人参皂苷Rh2 （Ginsenoside Rh2, Rh2）是一种中药活性化合物，具有抑制肿瘤细胞增殖和转移等抗癌作用。我们前期的研究发现，Rh2与IFNγ联合可增强癌细胞中CXCL10的分泌。在这里，我们探讨了Rh2和IFNγ是否在体外和体内发挥更有效的抗癌活性，以及其机制和临床价值。我们的数据显示，Rh2与IFNγ的结合导致HT29、LoVo和T84细胞系中结直肠癌细胞的细胞毒性显著增加。与此一致的是，瘤内注射Rh2 + IFNγ进一步限制了HT29肿瘤的体内生长，重要的是，它被证明对小鼠是安全的。同时，联合治疗激活癌细胞中干扰素基因刺激因子（STING）通路，促进下游I型干扰素的转录。RNA测序显示，与IFNγ单独治疗相比，Rh2进一步增强了干扰素信号通路的激活，在联合治疗的癌细胞中发生了显著的转录改变。ruxolitinib对janus激酶（JAK）的抑制作用可明显挽救联合治疗引起的细胞死亡。然后，定义了一个名为Rh2+IFNγ特征基因（RISG）的基因集，其中包含了联合治疗中前20个显著上调的基因。对免疫治疗有良好反应的患者与无反应的患者相比，肿瘤中RISG的表达更高。在结直肠癌（CRC）和皮肤黑色素瘤（SKCM）患者中，RISG的高表达与更好的临床预后相关。在本研究中，Rh2与IFNγ的结合是一种很有前景的癌症治疗策略，其衍生的RISG基因集在预测临床结果方面也显示出潜在的价值。Rh2联合IFNγ抗癌作用示意图。从原理图可以看出，人参皂苷Rh2与IFNγ结合，可以有效激活癌细胞中的干扰素信号，最终导致癌细胞显著死亡。isg，干扰素刺激基因。创建与BioRender.com。

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 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.