Wang Wei, Liu Xiangnan, Xu Shengjie, Dai Enci, Li Yingying, Liu Yinping, Shan Liyun, Li Yanli
Department of Obstetrics and Gynecology, Shanghai General Hospital, Shanghai Jiao Tong University School of Medicine, Shanghai, People's Republic of China.
Transl Oncol. 2025 Jul;57:102414. doi: 10.1016/j.tranon.2025.102414. Epub 2025 May 16.
Ovarian cancer, ranking fifth in cancer mortality, presents a significant therapeutic challenge. The immunomodulatory functions of CD38in epithelial ovarian cancer (EOC) and its influence on the tumor microenvironment (TME) remain poorly understood.
Public datasets, RT-qPCR and immunohistochemistry (IHC) were used to analyze CD38 expression and clinicopathological features in EOC. Gene manipulation techniques were employed to elucidate its functions, while integrated IHC and bioinformatics were conducted to assess its involvement in immune/stromal infiltration. Immune-related functions of CD38 were explored using GO, KEGG analysis and TIP database. TIDE algorithm was employed to predict the correlation between CD38 and immune checkpoint blocking responsiveness. CD38 inhibitor efficacy was evaluated in an EOC mouse model, with flow cytometry monitoring cellular changes. The involvement of CD38 in the PI3K-AKT and IL-6 signaling pathways was evaluated using RT-qPCR, western blot, and publicly datasets.
CD38 is significantly upregulated in EOC, influencing the cell proliferation and metastasis. It regulates the PI3K-AKT and IL-6 signaling pathways, thereby increasing tumor malignancy. CD38 is also upregulated in immune and stromal cells, affecting TME remodeling by facilitating immune cell and CAF infiltration, impeding T cell recognition of tumor cells, and enhancing CAF-tumor cell communication. Additionally, CD38 correlates with multiple immune checkpoint molecules. Notably, CD38 inhibitor therapy inhibited effectively EOC progression and modulates immune responses.
Elevated CD38 expression is associated with EOC progression, TME remodeling, and immune response modulation. Thus, CD38 could be a promising target for ovarian cancer immunotherapy.
卵巢癌的癌症死亡率排名第五,带来了重大的治疗挑战。CD38在上皮性卵巢癌(EOC)中的免疫调节功能及其对肿瘤微环境(TME)的影响仍知之甚少。
利用公共数据集、RT-qPCR和免疫组织化学(IHC)分析EOC中CD38的表达及临床病理特征。采用基因操作技术阐明其功能,同时进行综合IHC和生物信息学分析以评估其在免疫/基质浸润中的作用。使用GO、KEGG分析和TIP数据库探索CD38的免疫相关功能。采用TIDE算法预测CD38与免疫检查点阻断反应性之间的相关性。在EOC小鼠模型中评估CD38抑制剂的疗效,通过流式细胞术监测细胞变化。使用RT-qPCR、western blot和公共数据集评估CD38在PI3K-AKT和IL-6信号通路中的作用。
CD38在EOC中显著上调,影响细胞增殖和转移。它调节PI3K-AKT和IL-6信号通路,从而增加肿瘤恶性程度。CD38在免疫细胞和基质细胞中也上调,通过促进免疫细胞和CAF浸润、阻碍T细胞对肿瘤细胞的识别以及增强CAF-肿瘤细胞通讯来影响TME重塑。此外,CD38与多种免疫检查点分子相关。值得注意的是,CD38抑制剂治疗有效抑制了EOC进展并调节免疫反应。
CD38表达升高与EOC进展、TME重塑和免疫反应调节相关。因此,CD38可能是卵巢癌免疫治疗的一个有前景的靶点。
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