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Literature DB >> 30723143

Activated and Exhausted MAIT Cells Foster Disease Progression and Indicate Poor Outcome in Hepatocellular Carcinoma.

Meng Duan¹, Shyamal Goswami², Jie-Yi Shi¹, Lin-Jie Wu³, Xiao-Ying Wang¹, Jia-Qiang Ma², Zhao Zhang¹, Yang Shi⁴, Li-Jie Ma¹, Shu Zhang¹, Rui-Bin Xi^3,5, Ya Cao⁶, Jian Zhou^1,7,8, Jia Fan^9,7,8, Xiao-Ming Zhang¹⁰, Qiang Gao^9,8.

Abstract

PURPOSE: Innate immunity is an indispensable arm of tumor immune surveillance, and the liver is an organ with a predominance of innate immunity, where mucosal-associated invariant T (MAIT) cells are enriched. However, little is known about the phenotype, functions, and immunomodulatory role of MAIT cells in hepatocellular carcinoma (HCC).Experimental Design: The distribution, phenotype, and function of MAIT cells in patients with HCC were evaluated by both flow cytometry (FCM) and in vitro bioassays. Transcriptomic analysis of MAIT cells was also performed. Prognostic significance of tumor-infiltrating MAIT cells was validated in four independent cohorts of patients with HCC.
RESULTS: Despite their fewer densities in HCC tumor than normal liver, MAIT cells were significantly enriched in the HCC microenvironment compared with other mucosa-associated organs. Tumor-derived MAIT cells displayed a typical CCR7-CD45RA-CD45RO+CD95+ effector memory phenotype with lower costimulatory and effector capabilities. Tumor-educated MAIT cells significantly upregulated inhibitory molecules like PD-1, CTLA-4, TIM-3, secreted significantly less IFNγ and IL17, and produced minimal granzyme B and perforin while shifting to produce tumor-promoting cytokines like IL8. Transcriptome sequencing confirmed that tumor-derived MAIT cells were reprogrammed toward a tumor-promoting direction by downregulating genes enriched in pathways of cytokine secretion and cytolysis effector function like NFKB1 and STAT5B and by upregulating genes like IL8, CXCL12, and HAVCR2 (TIM-3). High infiltration of MAIT cells in HCC significantly correlated with an unfavorable clinical outcome, revealed by FCM, qRT-PCR, and multiplex IHC analyses, respectively.
CONCLUSIONS: HCC-infiltrating MAIT cells were functionally impaired and even reprogrammed to shift away from antitumor immunity and toward a tumor-promoting direction.See related commentary by Carbone, p. 3199. ©2019 American Association for Cancer Research.

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Year: 2019 PMID： 30723143 DOI： 10.1158/1078-0432.CCR-18-3040

Source DB: PubMed Journal: Clin Cancer Res ISSN： 1078-0432 Impact factor: 12.531

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Cited

40 in total

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Review 3. MAIT cells and their implication in human oral diseases.

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Review 4. Mucosal-associated invariant T cells and disease.

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Review 5. Immunobiology and immunotherapy of HCC: spotlight on innate and innate-like immune cells.

Authors: Benjamin Ruf; Bernd Heinrich; Tim F Greten
Journal: Cell Mol Immunol Date: 2020-11-24 Impact factor: 11.530

6. MAIT cells numbers and frequencies in patients with acute myeloid leukemia at diagnosis: association with cytogenetic profile and gene mutations.

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Journal: Cancer Immunol Immunother Date: 2021-09-03 Impact factor: 6.968

Review 7. Innate lymphocytes: pathogenesis and therapeutic targets of liver diseases and cancer.

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Review 8. Mouse models illuminate MAIT cell biology.

Authors: Huimeng Wang; Zhenjun Chen; James McCluskey; Alexandra J Corbett
Journal: Mol Immunol Date: 2020-12-22 Impact factor: 4.407

9. Activating Mucosal-Associated Invariant T Cells Induces a Broad Antitumor Response.

Authors: Benjamin Ruf; Vanessa V Catania; Simon Wabitsch; Chi Ma; Laurence P Diggs; Qianfei Zhang; Bernd Heinrich; Varun Subramanyam; Linda L Cui; Marie Pouzolles; Christine N Evans; Raj Chari; Shunsuke Sakai; Sangmi Oh; Clifton E Barry; Daniel L Barber; Tim F Greten
Journal: Cancer Immunol Res Date: 2021-06-30 Impact factor: 12.020

10. Functional inactivation of pulmonary MAIT cells following 5-OP-RU treatment of non-human primates.

Authors: Shunsuke Sakai; Nickiana E Lora; Keith D Kauffman; Danielle E Dorosky; Sangmi Oh; Sivaranjani Namasivayam; Felipe Gomez; Joel D Fleegle; Cecilia S Lindestam Arlehamn; Alessandro Sette; Alan Sher; Gordon J Freeman; Laura E Via; Clifton E Barry Iii; Daniel L Barber
Journal: Mucosal Immunol Date: 2021-06-22 Impact factor: 7.313