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Genomic mapping identifies mutations in ryr2 and ahnak as associated with favorable outcome in basal-like breast tumors expressing pd1/pd-l1
Cimas, F.J.
;
Manzano, A.
;
Baliu-Piqué, M.
;
García-Gil, E.
;
Pérez-Segura, P.
;
Nagy, Á. [Nagy, Ádám (biológia), author] Institute of Enzymology (RCNS); II. Department of Pediatrics (SU / FM / C); Bioinformatika Tanszék (SU / FM / I)
;
Pandiella, A.
;
Győrffy, B. [Győrffy, Balázs (Onkológia), author] II. Department of Pediatrics (SU / FM / C); Enzim_417 (IMLS); Bioinformatika Tanszék (SU / FM / I)
;
Ocana, A. ✉
English Article (Journal Article) Scientific
Published:
CANCERS 2072-6694
12
(8)
Paper: 2243
, 15 p.
2020
SJR Scopus - Oncology: Q1
Identifiers
MTMT: 31411617
DOI:
10.3390/cancers12082243
SE Repozitórium:
8487
REAL:
114054
WoS:
000579050800001
Scopus:
85089402503
PubMed:
32796628
Treatment with anti-PD-L1 antibodies has shown efficacy in basal-like breast cancer. In this context, identification of pre-activated immune tumors is a main goal. Here we explore mutations in PD1 and PD-L1 high-expressing tumors to identify genomic correlates associated with outcome. To do so, RNA-seq and mutation data from 971 breast cancer patients from the TCGA dataset were used to identify most prevalent mutations in patients with high levels of PD1 and PD-L1. Transcriptomic signatures associated with the selected mutations were identified and analyzed in terms of outcome and immune cell infiltration. We identified co-occurrent mutations in RYR2 and AHNAK in 8% and 5% of basal-like tumors respectively, which conferred good prognosis in patients with high expression of PD1 and PD-L1 genes. The transcriptomic signature associated with these mutations, composed of CXCL9, GBP5, C1QA, IL2RG, CSF2RB, IDO1 and LAG3 genes, also conferred good prognosis and correlated with immune infiltrations within the tumors. The joint signature classified patients with favorable relapse-free survival (HR: 0.28; CI: 0.2–0.38; p = 1.7 × 10−16) and overall survival (HR: 0.18; CI: 0.09–0.34; p = 6.8 × 10−9), showing a stronger prediction capacity than previous reported signatures. In conclusion, we describe two novel mutations and their transcriptomic signature, both associated with a favorable outcome and immune infiltrates in PD1 and PD-L1 high-expressing basal-like tumors. © 2020 by the authors. Licensee MDPI, Basel, Switzerland.
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2025-04-25 08:08
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