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Literature DB >> 35404405

Carbon Monoxide Activates PERK-Regulated Autophagy to Induce Immunometabolic Reprogramming and Boost Antitumor T-cell Function.

Paramita Chakraborty¹, Rasesh Y Parikh², Seungho Choi¹, Danh Tran¹, Monika Gooz³, Zachariah T Hedley¹, Do-Sung Kim¹, Dariusz Pytel^2,4, Inhong Kang⁵, Satish N Nadig¹, Gyda C Beeson³, Lauren Ball⁶, Meenal Mehrotra⁵, Hongjun Wang¹, Stefano Berto⁷, Viswanathan Palanisamy², Hong Li⁸, Shilpak Chatterjee¹, Paulo C Rodriguez⁹, Eduardo N Maldonado³, J Alan Diehl¹⁰, Vamsi K Gangaraju², Shikhar Mehrotra^1,11.

Abstract

Mitochondria and endoplasmic reticulum (ER) share structural and functional networks and activate well-orchestrated signaling processes to shape cells' fate and function. While persistent ER stress (ERS) response leads to mitochondrial collapse, moderate ERS promotes mitochondrial function. Strategies to boost antitumor T-cell function by targeting ER-mitochondria cross-talk have not yet been exploited. Here, we used carbon monoxide (CO), a short-lived gaseous molecule, to test whether engaging moderate ERS conditions can improve mitochondrial and antitumor functions in T cells. In melanoma antigen-specific T cells, CO-induced transient activation of ERS sensor protein kinase R-like endoplasmic reticulum kinase (PERK) significantly increased antitumor T-cell function. Furthermore, CO-induced PERK activation temporarily halted protein translation and induced protective autophagy, including mitophagy. The use of LC3-GFP enabled differentiation between the cells that prepare themselves to undergo active autophagy (LC3-GFPpos) and those that fail to enter the process (LC3-GFPneg). LC3-GFPpos T cells showed strong antitumor potential, whereas LC3-GFPneg cells exhibited a T regulatory-like phenotype, harbored dysfunctional mitochondria, and accumulated abnormal metabolite content. These anomalous ratios of metabolites rendered the cells with a hypermethylated state and distinct epigenetic profile, limiting their antitumor activity. Overall, this study shows that ERS-activated autophagy pathways modify the mitochondrial function and epigenetically reprogram T cells toward a superior antitumor phenotype to achieve robust tumor control. SIGNIFICANCE: Transient activation of ER stress with carbon monoxide drives mitochondrial biogenesis and protective autophagy that elicits superior antitumor T-cell function, revealing an approach to improving adoptive cell efficacy therapy. ©2022 American Association for Cancer Research.

Entities: Chemical

Mesh：

Substances：

Year: 2022 PMID： 35404405 PMCID： PMC9117468 DOI： 10.1158/0008-5472.CAN-21-3155

Source DB: PubMed Journal: Cancer Res ISSN： 0008-5472 Impact factor: 13.312

64 in total

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Journal: Methods Enzymol Date: 2011 Impact factor: 1.600

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Authors: Caroline Pot; Lionel Apetoh; Amit Awasthi; Vijay K Kuchroo
Journal: Semin Immunol Date: 2011-09-03 Impact factor: 11.130

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Authors: Roberto Bravo; Jose Miguel Vicencio; Valentina Parra; Rodrigo Troncoso; Juan Pablo Munoz; Michael Bui; Clara Quiroga; Andrea E Rodriguez; Hugo E Verdejo; Jorge Ferreira; Myriam Iglewski; Mario Chiong; Thomas Simmen; Antonio Zorzano; Joseph A Hill; Beverly A Rothermel; Gyorgy Szabadkai; Sergio Lavandero
Journal: J Cell Sci Date: 2011-05-31 Impact factor: 5.285

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Authors: Fangming Lin; Zhao V Wang; Joseph A Hill
Journal: Autophagy Date: 2014-01-14 Impact factor: 16.016

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Authors: Yukiko Iwasaki; Keishi Fujio; Tomohisa Okamura; Kazuhiko Yamamoto
Journal: Int J Mol Sci Date: 2015-01-27 Impact factor: 5.923

Review 6. Carbon monoxide and mitochondria-modulation of cell metabolism, redox response and cell death.

Authors: Ana S Almeida; Cláudia Figueiredo-Pereira; Helena L A Vieira
Journal: Front Physiol Date: 2015-02-09 Impact factor: 4.566

7. ER stress-induced mediator C/EBP homologous protein thwarts effector T cell activity in tumors through T-bet repression.

Authors: Yu Cao; Jimena Trillo-Tinoco; Rosa A Sierra; Carmen Anadon; Wenjie Dai; Eslam Mohamed; Ling Cen; Tara L Costich; Anthony Magliocco; Douglas Marchion; Richard Klar; Sven Michel; Frank Jaschinski; Richard R Reich; Shikhar Mehrotra; Juan R Cubillos-Ruiz; David H Munn; Jose R Conejo-Garcia; Paulo C Rodriguez
Journal: Nat Commun Date: 2019-03-20 Impact factor: 14.919

1. PERK promotes immunosuppressive M2 macrophage phenotype by metabolic reprogramming and epigenetic modifications through the PERK-ATF4-PSAT1 axis.

Authors: Uday P Pratap; Ratna K Vadlamudi
Journal: Immunometabolism (Cobham) Date: 2022-07-29

2. Significance of immunogenic cell death-related genes in prognosis prediction and immune microenvironment landscape of patients with cutaneous melanoma.

Authors: Weijiang Fu; Guangxin Ma
Journal: Front Genet Date: 2022-09-21 Impact factor: 4.772

2 in total