ALK peptide vaccination restores the immunogenicity of ALK-rearranged non-small cell lung cancer

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作者
Ines Mota
Enrico Patrucco
Cristina Mastini
Navin R. Mahadevan
Tran C. Thai
Elisa Bergaggio
Taek-Chin Cheong
Giulia Leonardi
Elif Karaca-Atabay
Marco Campisi
Teresa Poggio
Matteo Menotti
Chiara Ambrogio
Dario L. Longo
Susan Klaeger
Hasmik Keshishian
Zsófia M. Sztupinszki
Zoltan Szallasi
Derin B. Keskin
Jonathan S. Duke-Cohan
Bruce Reinhold
Steven A. Carr
Catherine J. Wu
Kelly D. Moynihan
Darrell J. Irvine
David A. Barbie
Ellis L. Reinherz
Claudia Voena
Mark M. Awad
Rafael B. Blasco
Roberto Chiarle
机构
[1] Boston Children’s Hospital,Department of Pathology
[2] University of Torino,Department of Molecular Biotechnology and Health Sciences
[3] Dana–Farber Cancer Institute,Department of Medical Oncology
[4] Brigham and Women’s Hospital,Department of Pathology
[5] University of Torino,Molecular Imaging Center
[6] National Research Council of Italy (CNR),Institute of Biostructures and Bioimaging (IBB)
[7] Broad Institute of MIT and Harvard,Computational Health Informatics Program
[8] Danish Cancer Society Research Center,Department of Bioinformatics
[9] Boston Children’s Hospital,Translational Immunogenomics Laboratory
[10] Semmelweis University,Department of Computer Science, Metropolitan College
[11] Dana–Farber Cancer Institute,Section for Bioinformatics, Department of Health Technology
[12] Boston University,Laboratory of Immunobiology
[13] Technical University of Denmark,Department of Medicine
[14] Dana–Farber Cancer Institute,Koch Institute for Integrative Cancer Research
[15] Brigham and Women’s Hospital,undefined
[16] Massachusetts Institute of Technology,undefined
[17] Howard Hughes Medical Institute,undefined
来源
Nature Cancer | 2023年 / 4卷
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摘要
Anaplastic lymphoma kinase (ALK)-rearranged non-small cell lung cancer (NSCLC) is treated with ALK tyrosine kinase inhibitors (TKIs), but the lack of activity of immune checkpoint inhibitors (ICIs) is poorly understood. Here, we identified immunogenic ALK peptides to show that ICIs induced rejection of ALK+ tumors in the flank but not in the lung. A single-peptide vaccination restored priming of ALK-specific CD8+ T cells, eradicated lung tumors in combination with ALK TKIs and prevented metastatic dissemination of tumors to the brain. The poor response of ALK+ NSCLC to ICIs was due to ineffective CD8+ T cell priming against ALK antigens and is circumvented through specific vaccination. Finally, we identified human ALK peptides displayed by HLA-A*02:01 and HLA-B*07:02 molecules. These peptides were immunogenic in HLA-transgenic mice and were recognized by CD8+ T cells from individuals with NSCLC, paving the way for the development of a clinical vaccine to treat ALK+ NSCLC.
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页码:1016 / 1035
页数:19
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