Spatial heterogeneity of the T cell receptor repertoire reflects the mutational landscape in lung cancer

被引:0
|
作者
Kroopa Joshi
Marc Robert de Massy
Mazlina Ismail
James L. Reading
Imran Uddin
Annemarie Woolston
Emine Hatipoglu
Theres Oakes
Rachel Rosenthal
Thomas Peacock
Tahel Ronel
Mahdad Noursadeghi
Virginia Turati
Andrew J. S. Furness
Andrew Georgiou
Yien Ning Sophia Wong
Assma Ben Aissa
Mariana Werner Sunderland
Mariam Jamal-Hanjani
Selvaraju Veeriah
Nicolai J. Birkbak
Gareth A. Wilson
Crispin T. Hiley
Ehsan Ghorani
José Afonso Guerra-Assunção
Javier Herrero
Tariq Enver
Sine R. Hadrup
Allan Hackshaw
Karl S. Peggs
Nicholas McGranahan
Charles Swanton
Sergio A. Quezada
Benny Chain
机构
[1] University College London Cancer Institute,Cancer Immunology Unit, Research Department of Haematology
[2] The Royal Marsden NHS Foundation Trust,Department of Medical Oncology
[3] University College London,Division of Infection and Immunity
[4] University College London Cancer Institute,Cancer Research UK Lung Cancer Centre of Excellence
[5] University College London Cancer Institute,Bill Lyons Informatics Centre
[6] University College London,Computation, Mathematics and Physics in the Life Sciences and Experimental Biology, Department of Computer Science
[7] University College London Cancer Institute,Department of Cancer Biology
[8] The Francis Crick Institute,Cancer Evolution and Genome Instability Laboratory
[9] University College London Cancer Institute,Department of Health Technology
[10] Technical University of Denmark,Department of Computer Sciences
[11] University College London,Cancer Research UK Manchester Institute
[12] Cancer Research UK & UCL Cancer Trials Centre,Cancer Research UK Lung Cancer Centre of Excellence
[13] The Francis Crick Institute,Division of Infection, Immunity and Respiratory Medicine
[14] University College London Hospitals,Cancer Research Centre
[15] Aberdeen Royal Infirmary,Department of Physics of Complex Systems
[16] Ashford and St Peter’s Hospitals NHS Foundation Trust,Department of Radiology
[17] Barnet Hospital and Chase Farm Hospital,undefined
[18] Barts Health NHS Trust,undefined
[19] Berlin Institute for Medical Systems Biology,undefined
[20] Max Delbrueck Center for Molecular Medicine,undefined
[21] German Cancer Consortium (DKTK),undefined
[22] partner site Berlin,undefined
[23] German Cancer Research Center (DKFZ),undefined
[24] University of Manchester,undefined
[25] University of Manchester,undefined
[26] Christie NHS Foundation Trust,undefined
[27] Wythenshawe Hospital,undefined
[28] Manchester University NHS Foundation Trust,undefined
[29] University of Manchester,undefined
[30] University of Leicester,undefined
[31] Leicester University Hospitals,undefined
[32] Cardiff & Vale University Health Board,undefined
[33] Danish Cancer Society Research Center,undefined
[34] Department of Pathology,undefined
[35] GZA-ZNA Antwerp,undefined
[36] ELTE Eötvös Loránd University,undefined
[37] Departments of Radiation Oncology and Radiology,undefined
[38] Dana-Farber Cancer Institute,undefined
[39] Brigham and Women’s Hospital,undefined
[40] Harvard Medical School,undefined
[41] Netherlands Cancer Institute,undefined
[42] Golden Jubilee National Hospital,undefined
[43] Independent Cancer Patients’ Voice,undefined
[44] University of Leicester,undefined
[45] Liverpool Heart and Chest Hospital NHS Foundation Trust,undefined
[46] Royal Liverpool University Hospital,undefined
[47] Manchester Cancer Research Centre Biobank,undefined
[48] National Institute for Health Research Leicester Respiratory Biomedical Research Unit,undefined
[49] NHS Greater Glasgow and Clyde,undefined
[50] Royal Brompton and Harefield NHS Foundation Trust,undefined
来源
Nature Medicine | 2019年 / 25卷
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摘要
Somatic mutations together with immunoediting drive extensive heterogeneity within non-small-cell lung cancer (NSCLC). Herein we examine heterogeneity of the T cell antigen receptor (TCR) repertoire. The number of TCR sequences selectively expanded in tumors varies within and between tumors and correlates with the number of nonsynonymous mutations. Expanded TCRs can be subdivided into TCRs found in all tumor regions (ubiquitous) and those present in a subset of regions (regional). The number of ubiquitous and regional TCRs correlates with the number of ubiquitous and regional nonsynonymous mutations, respectively. Expanded TCRs form part of clusters of TCRs of similar sequence, suggestive of a spatially constrained antigen-driven process. CD8+ tumor-infiltrating lymphocytes harboring ubiquitous TCRs display a dysfunctional tissue-resident phenotype. Ubiquitous TCRs are preferentially detected in the blood at the time of tumor resection as compared to routine follow-up. These findings highlight a noninvasive method to identify and track relevant tumor-reactive TCRs for use in adoptive T cell immunotherapy.
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页码:1549 / 1559
页数:10
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