BACH2 enforces the transcriptional and epigenetic programs of stem-like CD8+ T cells

被引:0
|
作者
Chen Yao
Guohua Lou
Hong-Wei Sun
Ziang Zhu
Yi Sun
Zeyu Chen
Daniel Chauss
E. Ashley Moseman
Jun Cheng
Marc A. D’Antonio
Wangke Shi
Junwei Shi
Kohei Kometani
Tomohiro Kurosaki
E. John Wherry
Behdad Afzali
Luca Gattinoni
Yuwen Zhu
Dorian B. McGavern
John J. O’Shea
Pamela L. Schwartzberg
Tuoqi Wu
机构
[1] National Institute of Arthritis and Musculoskeletal and Skin Diseases,Molecular Immunology and Inflammation Branch
[2] National Institutes of Health,Department of Immunology and Microbiology
[3] University of Colorado Anschutz Medical Campus,Department of Surgery, Division of Surgical Oncology
[4] University of Colorado Anschutz Medical Campus,Department of Systems Pharmacology and Translational Therapeutics
[5] University of Pennsylvania Perelman School Medicine,Immunoregulation Section, Kidney Diseases Branch
[6] National Institute of Diabetes and Digestive and Kidney Diseases,Department of Immunology
[7] National Institutes of Health,Department of Cancer Biology
[8] Duke University School of Medicine,Laboratory of Lymphocyte Differentiation
[9] National Human Genome Research Institute,Laboratory of Lymphocyte Differentiation
[10] National Institutes of Health,Regensburg Center for Interventional Immunology
[11] University of Pennsylvania Perelman School Medicine,Viral Immunology and Intravital Imaging Section
[12] RIKEN Center for Integrative Medical Sciences (IMS),Laboratory of Immune System Biology
[13] WPI Immunology Frontier Research Center,undefined
[14] Osaka University,undefined
[15] University of Regensburg,undefined
[16] National Institute of Neurological Disorders and Stroke,undefined
[17] National Institutes of Health,undefined
[18] National Institute of Allergy and Infectious Diseases,undefined
[19] National Institutes of Health,undefined
来源
Nature Immunology | 2021年 / 22卷
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摘要
During chronic infection and cancer, a self-renewing CD8+ T cell subset maintains long-term immunity and is critical to the effectiveness of immunotherapy. These stem-like CD8+ T cells diverge from other CD8+ subsets early after chronic viral infection. However, pathways guarding stem-like CD8+ T cells against terminal exhaustion remain unclear. Here, we show that the gene encoding transcriptional repressor BACH2 is transcriptionally and epigenetically active in stem-like CD8+ T cells but not terminally exhausted cells early after infection. BACH2 overexpression enforced stem-like cell fate, whereas BACH2 deficiency impaired stem-like CD8+ T cell differentiation. Single-cell transcriptomic and epigenomic approaches revealed that BACH2 established the transcriptional and epigenetic programs of stem-like CD8+ T cells. In addition, BACH2 suppressed the molecular program driving terminal exhaustion through transcriptional repression and epigenetic silencing. Thus, our study reveals a new pathway that enforces commitment to stem-like CD8+ lineage and prevents an alternative terminally exhausted cell fate.
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页码:370 / 380
页数:10
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