Molecular profiling of long-term responders to immune checkpoint inhibitors in advanced non-small cell lung cancer

dc.contributor.author
Frigola Rissech, Joan
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Navarro, Alejandro
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Carbonell, Caterina
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Callejo, Ana
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Iranzo, Patricia
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Cedrés, Susana
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Martinez-Marti, Alex
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Pardo Aranda, Nuria
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Saoudi-Gonzalez, Nadia
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Martínez, Débora
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Jiménez, José
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Sansano, Irene
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Mancuso, Francesco M.
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Nuciforo, Paolo
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Montuenga, Luis M.
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Sanchez-Cespedes, Montse
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Prat, Aleix
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Vivancos, Ana
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Felip, Enriqueta
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Amat, Ramon
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Universitat Autònoma de Barcelona
dc.date.issued
2020
dc.identifier
https://ddd.uab.cat/record/236714
dc.identifier
urn:10.1002/1878-0261.12891
dc.identifier
urn:oai:ddd.uab.cat:236714
dc.identifier
urn:scopus_id:85099016399
dc.identifier
urn:pmid:33342055
dc.identifier
urn:pmc-uid:8024716
dc.identifier
urn:pmcid:PMC8024716
dc.identifier
urn:oai:pubmedcentral.nih.gov:8024716
dc.identifier
urn:oai:egreta.uab.cat:publications/5690b345-9beb-4629-9659-16c434a13999
dc.description.abstract
Altres ajuts: This work was supported by the Fundacion Cientifica Asociación Española Contra el Cancer-AECC [grant number GCB14142170 to LMM, MS-C, and EF].
dc.description.abstract
Immunotherapy has transformed advanced non-small cell lung cancer (NSCLC) treatment strategies and has led to unprecedented long-lasting responses in some patients. However, the molecular determinants driving these long-term responses remain elusive. To address this issue, we performed an integrative analysis of genomic and transcriptomic features of long-term immune checkpoint inhibitors (ICIs)-associated responders. We assembled a cohort of 47 patients with NSCLC receiving ICIs that was enriched in long-term responders [>18 months of progression-free survival (PFS)]. We performed whole-exome sequencing from tumor samples, estimated the tumor mutational burden (TMB), and inferred the somatic copy number alterations (SCNAs). We also obtained gene transcription data for a subset of patients using Nanostring, which we used to assess the tumor immune infiltration status and PD-L1 expression. Our results indicate that there is an association between TMB and benefit to ICIs, which is driven by those patients with long-term response. Additionally, high SCNAs burden is associated with poor response and negatively correlates with the presence of several immune cell types (B cells, natural killers, regulatory T cells or effector CD8 T cells). Also, CD274 (PD-L1) expression is increased in patients with benefit, mainly in those with long-term response. In our cohort, combined assessment of TMB and SCNAs burden enabled identification of long-term responders (considering PFS and overall survival). Notably, the association between TMB, SCNAs burden, and PD-L1 expression with the outcomes of ICIs treatment was validated in two public datasets of ICI-treated patients with NSCLC. Thus, our data indicate that TMB is associated with long-term benefit following ICIs treatment in NSCLC and that TMB, SCNAs burden, and PD-L1 are complementary determinants of response to ICIs.
dc.format
application/pdf
dc.language
eng
dc.publisher
dc.relation
Agència de Gestió d'Ajuts Universitaris i de Recerca 2017/SGR-1738
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Instituto de Salud Carlos III PI17-00938
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Molecular oncology ; 2020
dc.rights
open access
dc.rights
Aquest document està subjecte a una llicència d'ús Creative Commons. Es permet la reproducció total o parcial, la distribució, la comunicació pública de l'obra i la creació d'obres derivades, fins i tot amb finalitats comercials, sempre i quan es reconegui l'autoria de l'obra original.
dc.rights
https://creativecommons.org/licenses/by/4.0/
dc.subject
NSCLC
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PD-L1
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Chromosomal alterations burden
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Copy number alterations
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Immune checkpoint inhibitors
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Long-term benefit
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Tumor mutational burden
dc.title
Molecular profiling of long-term responders to immune checkpoint inhibitors in advanced non-small cell lung cancer
dc.type
Article


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