单细胞RNA测序揭示癌症相关成纤维细胞PTN在乙型肝炎病毒肝硬化-肝癌进展中的介导作用。
Single-cell RNA sequencing reveals the mediatory role of cancer-associated fibroblast PTN in hepatitis B virus cirrhosis-HCC progression.
作者信息
Lin Chenhong, Chen Yeda, Zhang Feng, Zhu Peng, Yu Liangliang, Chen Wenbiao
机构信息
Department of Endoscopy Center, Sir Run Run Shaw Hospital, Zhejiang University School of Medicine, Hangzhou, 310000, China.
Central Laboratory, People's Hospital of Longhua, The Affiliated Hospital of Southern Medical University, Shenzhen, 518109, China.
出版信息
Gut Pathog. 2023 May 31;15(1):26. doi: 10.1186/s13099-023-00554-z.
BACKGROUND
Cancer-associated fibroblasts (CAFs) are essential stromal components in the tumor microenvironment of hepatocellular carcinoma (HCC). Hepatitis B virus (HBV) infection induces pathological changes such as liver fibrosis/cirrhosis and HCC. The aim of this research was to explore the novel mediators of CAFs to modulate HBV cirrhosis-HCC progression.
METHODS
The single-cell transcriptome data of HCC were divided into subsets, and the significant subset related to fibrotic cells, along with biological function, and clinical information of HCC was revealed by integrated data analyses. The cell communication, cells communicated weight analysis of signaling pathways, and key genes in signaling pathways analysis of significant CAFs subclasses were conducted to discover the novel gene of CAFs. Bioinformatics, vitro and HBV transfection assays were used to verify the novel gene is an important target for promoting the progression HBV cirrhosis-HCC progression.
RESULTS
Fibroblasts derived from HCC single-cell data could be separated into three cell subclasses (CAF0-2), of which CAF2 was associated with the HCC clinical information. Fibroblasts have opposite developmental trajectories to immune B cells and CD8 + T cells. CAF0-2 had strong interaction with B cells and CD8 + T cells, especially CAF2 had the highest interaction frequency and weight with B cells and CD8 + T cells. Moreover, PTN participated in CAF2-related pathways involved in the regulation of cell communication, and the interactions among CAF2 and PTN contributed the most to B cells and CD8 + T cells. Furthermore, the genes of PTN, SDC1, and NCL from PTN signaling were highest expression in CAF2, B cells, and CD8 + T cells, respectively, and the interaction of PTN- SDC1 and PTN- NCL contributed most to the interaction of CAF2- B cells and CAF2-CD8 + T cells. Bioinformatics and vitro experiments confirm PTN was upregulated in HCC and promoted the proliferation of tumor cells, and HBV infection could initiate PTN to perform cirrhosis-HCC progression.
CONCLUSION
Our findings revealed CAF was associated with hepatocarcinogenesis, and the functional importance of B cells and CD8 + T cells in modulating CAF in HCC. Importantly, PTN maybe a novel mediator of CAF to mediate HBV cirrhosis-HCC progression.
背景
癌症相关成纤维细胞(CAFs)是肝细胞癌(HCC)肿瘤微环境中的重要基质成分。乙型肝炎病毒(HBV)感染会引发肝纤维化/肝硬化和HCC等病理变化。本研究的目的是探索CAFs调节HBV肝硬化 - HCC进展的新介质。
方法
将HCC的单细胞转录组数据分为子集,通过综合数据分析揭示与纤维化细胞相关的重要子集以及HCC的生物学功能和临床信息。对重要CAFs亚类进行细胞通讯、信号通路的细胞通讯权重分析以及信号通路中的关键基因分析,以发现CAFs的新基因。采用生物信息学、体外实验和HBV转染实验来验证该新基因是促进HBV肝硬化 - HCC进展的重要靶点。
结果
从HCC单细胞数据中分离出的成纤维细胞可分为三个细胞亚类(CAF0 - 2),其中CAF2与HCC临床信息相关。成纤维细胞与免疫B细胞和CD8 + T细胞具有相反的发育轨迹。CAF0 - 2与B细胞和CD8 + T细胞有强烈的相互作用,尤其是CAF2与B细胞和CD8 + T细胞的相互作用频率和权重最高。此外,PTN参与了与CAF2相关的细胞通讯调节途径,并且CAF2与PTN之间的相互作用对B细胞和CD8 + T细胞的影响最大。此外,PTN信号通路中的PTN、SDC1和NCL基因分别在CAF2、B细胞和CD8 + T细胞中表达最高,并且PTN - SDC1和PTN - NCL的相互作用对CAF2 - B细胞和CAF2 - CD8 + T细胞的相互作用贡献最大。生物信息学和体外实验证实PTN在HCC中上调并促进肿瘤细胞增殖,并且HBV感染可启动PTN促进肝硬化 - HCC进展。
结论
我们的研究结果揭示了CAF与肝癌发生相关,以及B细胞和CD8 + T细胞在调节HCC中CAF的功能重要性。重要的是,PTN可能是CAF介导HBV肝硬化 - HCC进展的新介质。
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