Tumor-specific cholinergic CD4+ T lymphocytes guide immunosurveillance of hepatocellular carcinoma

被引:0
|
作者
Chunxing Zheng
Bryan E. Snow
Andrew J. Elia
Robert Nechanitzky
Carmen Dominguez-Brauer
Shaofeng Liu
Yin Tong
Maureen A. Cox
Enrico Focaccia
Andrew C. Wakeham
Jillian Haight
Chantal Tobin
Kelsey Hodgson
Kyle T. Gill
Wei Ma
Thorsten Berger
Mathias Heikenwälder
Mary E. Saunders
Jerome Fortin
Suet Yi Leung
Tak W. Mak
机构
[1] University Health Network,Princess Margaret Cancer Centre
[2] Hong Kong Science Park,Centre for Oncology and Immunology
[3] University Health Network,Tumor Immunotherapy Program, Princess Margaret Cancer Centre
[4] The University of Hong Kong,Department of Pathology, School of Clinical Medicine, Li Ka Shing Faculty of Medicine
[5] Queen Mary Hospital,Division of Chronic Inflammation and Cancer
[6] Pokfulam,The M3 Research Center
[7] German Cancer Research Center (DKFZ),Departments of Immunology and Medical Biophysics
[8] Medical Faculty Tübingen,Department of Microbiology and Immunology
[9] University of Toronto,undefined
[10] University of Oklahoma Health Sciences Center,undefined
来源
Nature Cancer | 2023年 / 4卷
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摘要
Cholinergic nerves are involved in tumor progression and dissemination. In contrast to other visceral tissues, cholinergic innervation in the hepatic parenchyma is poorly detected. It remains unclear whether there is any form of cholinergic regulation of liver cancer. Here, we show that cholinergic T cells curtail the development of liver cancer by supporting antitumor immune responses. In a mouse multihit model of hepatocellular carcinoma (HCC), we observed activation of the adaptive immune response and induction of two populations of CD4+ T cells expressing choline acetyltransferase (ChAT), including regulatory T cells and dysfunctional PD-1+ T cells. Tumor antigens drove the clonal expansion of these cholinergic T cells in HCC. Genetic ablation of Chat in T cells led to an increased prevalence of preneoplastic cells and exacerbated liver cancer due to compromised antitumor immunity. Mechanistically, the cholinergic activity intrinsic in T cells constrained Ca2+–NFAT signaling induced by T cell antigen receptor engagement. Without this cholinergic modulation, hyperactivated CD25+ T regulatory cells and dysregulated PD-1+ T cells impaired HCC immunosurveillance. Our results unveil a previously unappreciated role for cholinergic T cells in liver cancer immunobiology.
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页码:1437 / 1454
页数:17
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