Function of mast cell and bile-cholangiocarcinoma interplay in cholangiocarcinoma microenvironment.

IF 23 1区 医学 Q1 GASTROENTEROLOGY & HEPATOLOGY
Gut Pub Date : 2024-07-11 DOI:10.1136/gutjnl-2023-331715
Anda Shi, Zengli Liu, Zhongqi Fan, Kangshuai Li, Xingkai Liu, Yongchang Tang, Jiaming Hu, Xingyong Li, Lizhuang Shu, Liming Zhao, Lingling Huang, Zhiyue Zhang, Guoyue Lv, Zongli Zhang, Yunfei Xu
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引用次数: 0

Abstract

Objective: The correlation between cholangiocarcinoma (CCA) progression and bile is rarely studied. Here, we aimed to identify differential metabolites in benign and malignant bile ducts and elucidate the generation, function and degradation of bile metabolites.

Design: Differential metabolites in the bile from CCA and benign biliary stenosis were identified by metabonomics. Biliary molecules able to induce mast cell (MC) degranulation were revealed by in vitro and in vivo experiments, including liquid chromatography-mass spectrometry (MS)/MS and bioluminescence resonance energy transfer assays. Histamine (HA) receptor expression in CCA was mapped using a single-cell mRNA sequence. HA receptor functions were elucidated by patient-derived xenografts (PDX) in humanised mice and orthotopic models in MC-deficient mice. Genes involved in HA-induced proliferation were screened by CRISPR/Cas9.

Results: Bile HA was elevated in CCA and indicated poorer prognoses. Cancer-associated fibroblasts (CAFs)-derived stem cell factor (SCF) recruited MCs, and bile N,N-dimethyl-1,4-phenylenediamine (DMPD) stimulated MCs to release HA through G protein-coupled receptor subtype 2 (MRGPRX2)-Gαq signalling. Bile-induced MCs released platelet-derived growth factor subunit B (PDGF-B) and angiopoietin 1/2 (ANGPT1/2), which enhanced CCA angiogenesis and lymphangiogenesis. Histamine receptor H1 (HRH1) and HRH2 were predominantly expressed in CCA cells and CAFs, respectively. HA promoted CCA cell proliferation by activating HRH1-Gαq signalling and hastened CAFs to secrete hepatocyte growth factor by stimulating HRH2-Gαs signalling. Solute carrier family 22 member 3 (SLC22A3) inhibited HA-induced CCA proliferation by importing bile HA into cells for degradation, and SLC22A3 deletion resulted in HA accumulation.

Conclusion: Bile HA is released from MCs through DMPD stimulation and degraded via SLC22A3 import. Different HA receptors exhibit a distinct expression profile in CCA and produce different oncogenic effects. MCs promote CCA progression in a CCA-bile interplay pattern.

胆管癌微环境中肥大细胞和胆汁-胆管癌相互作用的功能。
目的:胆管癌(CCA)进展与胆汁之间的相关性研究很少。在此,我们旨在确定良性和恶性胆管中的不同代谢物,并阐明胆汁代谢物的生成、功能和降解:设计:通过代谢组学鉴定CCA和良性胆道狭窄胆汁中的差异代谢物。通过体外和体内实验,包括液相色谱-质谱(MS)/MS和生物发光共振能量转移实验,揭示了能诱导肥大细胞(MC)脱颗粒的胆汁分子。利用单细胞 mRNA 序列绘制了组胺(HA)受体在 CCA 中的表达图。通过人源化小鼠的患者异种移植(PDX)和MC缺陷小鼠的正位模型阐明了HA受体的功能。通过CRISPR/Cas9筛选了参与HA诱导增殖的基因:结果:胆汁 HA 在 CCA 中升高,预后较差。癌症相关成纤维细胞(CAFs)衍生的干细胞因子(SCF)招募了MCs,胆汁中的N,N-二甲基-1,4-苯二胺(DMPD)通过G蛋白偶联受体亚型2(MRGPRX2)-Gαq信号刺激MCs释放HA。胆汁诱导的 MCs 释放血小板衍生生长因子亚基 B(PDGF-B)和血管生成素 1/2(ANGPT1/2),这增强了 CCA 的血管生成和淋巴管生成。组胺受体H1(HRH1)和HRH2分别在CCA细胞和CAFs中主要表达。HA通过激活HRH1-Gαq信号促进CCA细胞增殖,通过刺激HRH2-Gαs信号加速CAFs分泌肝细胞生长因子。溶质运载家族 22 成员 3(SLC22A3)通过将胆汁 HA 导入细胞降解来抑制 HA 诱导的 CCA 增殖,SLC22A3 缺失会导致 HA 积累:结论:胆汁HA通过DMPD刺激从MC释放,并通过SLC22A3导入降解。不同的 HA 受体在 CCA 中表现出不同的表达谱,并产生不同的致癌作用。MCs以CCA-胆汁相互作用的模式促进CCA的进展。
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
Gut
Gut 医学-胃肠肝病学
CiteScore
45.70
自引率
2.40%
发文量
284
审稿时长
1.5 months
期刊介绍: Gut is a renowned international journal specializing in gastroenterology and hepatology, known for its high-quality clinical research covering the alimentary tract, liver, biliary tree, and pancreas. It offers authoritative and current coverage across all aspects of gastroenterology and hepatology, featuring articles on emerging disease mechanisms and innovative diagnostic and therapeutic approaches authored by leading experts. As the flagship journal of BMJ's gastroenterology portfolio, Gut is accompanied by two companion journals: Frontline Gastroenterology, focusing on education and practice-oriented papers, and BMJ Open Gastroenterology for open access original research.
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