CCL28在肺腺癌免疫治疗中的综合探索及实验验证
Comprehensive Explorations of CCL28 in Lung Adenocarcinoma Immunotherapy and Experimental Validation.
作者信息
Su Xiangyu, Wang Guoqing, Zheng Shiya, Ge Chang, Kong Fei, Wang Cailian
机构信息
School of Medicine, Southeast University, Nanjing, 210009, People's Republic of China.
Department of Oncology, Zhongda Hospital, School of Medicine, Southeast University, Nanjing, 210009, People's Republic of China.
出版信息
J Inflamm Res. 2023 Mar 27;16:1325-1342. doi: 10.2147/JIR.S399193. eCollection 2023.
BACKGROUND
Chemokines have been reported to play an important role in cancer immunotherapy. This study aimed to explore the chemokines involved in lung cancer immunotherapy.
METHODS
All the public data were downloaded from The Cancer Genome Atlas Program database. Quantitative real time-PCR was used to detect the mRNA level of specific molecules and Western blot was used for the protein level. Other experiments used include luciferase reporter experiments, flow cytometric analysis, Chromatin immunoprecipitation assay, ELISA and co-cultured system.
RESULTS
We found that the CCL7, CCL11, CCL14, CCL24, CCL25, CCL26, CCL28 had a higher level, while the CCL17, CCL23 had a lower level in immunotherapy non-responders. Also, we found that immunotherapy non-responders had a higher level of CD56dim NK cells, NK cells, Th1 cells, Th2 cells and Treg, yet a lower level of iDC and Th17 cells. Biological enrichment analysis indicated that in the patients with high Treg infiltration, the pathways of pancreas beta cells, KRAS signaling, coagulation, WNT BETA catenin signaling, bile acid metabolism, interferon alpha response, hedgehog signaling, PI3K/AKT/mTOR signaling, apical surface, myogenesis were significantly enriched in. CCL7, CCL11, CCL26 and CCL28 were selected for further analysis. Compared with the patients with high CCL7, CCL11, CCL26 and CCL28 expression, the patients with low CCL7, CCL11, CCL26 and CCL28 expression had a better performance of immunotherapy response and this effect might partly be due to Treg cells. Furthermore, biological exploration and clinical correlation of CCL7, CCL11, CCL26 and CCL28 were conducted, Finally, CCL28 was selected for validation. Experiments showed that under the hypoxia condition, HIF-1α was upregulated, which can directly bind to the promoter region of CCL28 and lead to its higher level. Also, CCL28 secreted by lung cancer cells could induce Tregs infiltration.
CONCLUSION
Our study provides a novel insight focused on the chemokines in lung cancer immunotherapy. Also, CCL28 was identified as an underlying biomarker for lung cancer immunotherapy.
背景
据报道,趋化因子在癌症免疫治疗中发挥重要作用。本研究旨在探索肺癌免疫治疗中涉及的趋化因子。
方法
所有公共数据均从癌症基因组图谱计划数据库下载。采用定量实时聚合酶链反应检测特定分子的mRNA水平,采用蛋白质印迹法检测蛋白质水平。其他使用的实验包括荧光素酶报告基因实验、流式细胞术分析、染色质免疫沉淀分析、酶联免疫吸附测定和共培养系统。
结果
我们发现,在免疫治疗无反应者中,CCL7、CCL11、CCL14、CCL24、CCL25、CCL26、CCL28水平较高,而CCL17、CCL23水平较低。此外,我们发现免疫治疗无反应者的CD56dim自然杀伤(NK)细胞、NK细胞、辅助性T细胞1(Th1)、辅助性T细胞2(Th2)和调节性T细胞(Treg)水平较高,而未成熟树突状细胞(iDC)和辅助性T细胞17(Th17)水平较低。生物富集分析表明,在Treg浸润高的患者中,胰腺β细胞、KRAS信号传导、凝血、WNTβ连环蛋白信号传导、胆汁酸代谢、干扰素α反应、刺猬信号传导、磷脂酰肌醇-3激酶/蛋白激酶B/哺乳动物雷帕霉素靶蛋白(PI3K/AKT/mTOR)信号传导、顶端表面、肌生成等通路显著富集。选择CCL7、CCL11、CCL26和CCL28进行进一步分析。与CCL7、CCL11、CCL26和CCL28高表达的患者相比,CCL7、CCL11、CCL26和CCL28低表达的患者免疫治疗反应表现更好,且这种效应可能部分归因于Treg细胞。此外,对CCL7、CCL11、CCL26和CCL28进行了生物学探索和临床相关性分析,最后选择CCL28进行验证。实验表明,在缺氧条件下,低氧诱导因子-1α(HIF-1α)上调,其可直接结合CCL28的启动子区域并导致其水平升高。此外,肺癌细胞分泌的CCL28可诱导Treg浸润。
结论
我们的研究为肺癌免疫治疗中的趋化因子提供了新的见解。此外,CCL28被确定为肺癌免疫治疗的潜在生物标志物。
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