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dc.contributor.authorIngebriktsen, Lise Martine
dc.contributor.authorSvanøe, Amalie Abrahamsen
dc.contributor.authorSæle, Anna Kristine Myrmel
dc.contributor.authorHumlevik, Rasmus Olai Collett
dc.contributor.authorToska, Karen
dc.contributor.authorKalvenes, May Britt
dc.contributor.authorAas, Turid
dc.contributor.authorHeie, Anette
dc.contributor.authorAskeland, Cecilie
dc.contributor.authorKnutsvik, Gøril
dc.contributor.authorStefansson, Ingunn Marie
dc.contributor.authorAkslen, Lars Andreas
dc.contributor.authorHøivik, Erling André
dc.contributor.authorWik, Elisabeth
dc.date.accessioned2024-11-11T15:01:27Z
dc.date.available2024-11-11T15:01:27Z
dc.date.created2024-06-26T15:46:56Z
dc.date.issued2024
dc.identifier.issn0893-3952
dc.identifier.urihttps://hdl.handle.net/11250/3164425
dc.description.abstractBreast cancer (BC) patients aged <40 years at diagnosis experience aggressive disease and poorer survival compared with women diagnosed with BC at 40 to 49 years, but the age-related biology is described to little extent. Here, we explored transcriptional alterations in BC to gain better understanding of age-related tumor biology. We studied a subset of the Bergen in-house cohort (n = 127; age range, 26-49 years) and used the NanoString Breast Cancer 360 expression panel on formalin-fixed paraffin-embedded BC tissue, and publicly available global BC messenger RNA expression data (n = 204; age range, 22-49 years), to explore differentially expressed genes between the young (age <40 years) and older (age 40-49 years) patients. Unsupervised hierarchical clustering was applied to identify gene expression–based patient clusters. We applied established computational approaches to define the PAM50 subtypes, risk of recurrence scores (ROR), and risk groups and to infer the proportions of 22 immune cell types from bulk gene expression profiles of patients aged <50 years at BC diagnosis. Differentially expressed genes and gene sets were investigated using OncoEnrichR and g:Profiler to describe functional profiles and pathway enrichment. We identified 4 age-related patient clusters presenting distinct characteristics of PAM50 subtypes and ROR profiles, which demonstrated independent prognostic value when adjusted for traditional clinicopathologic variables and the known molecular subtypes. Our findings showed better survival than expected in the basal-enriched cluster 2 and in triple-negative and basal-like BC. Deconvolution analyses of immunophenotypes indicated higher levels of M0 and M1 macrophages than M2 macrophages in subsets of young BC. Our approach identifies age-based patient clusters with distinct clinicopathologic profiles, to a large extent overlapping with the PAM50 subtypes, although with independent prognostic values in multivariate survival analyses. The patient clusters provided new insight in the immune cell distribution across tumor subtypes, potentially contributing to survival differences between the clusters and the molecular subtypes and indicating age-related mechanisms improving outcome. Our study confirms the applicability of ROR as a valid prognosticator also in a young BC cohort.en_US
dc.language.isoengen_US
dc.publisherElsevieren_US
dc.rightsNavngivelse 4.0 Internasjonal*
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/deed.no*
dc.titleAge-Related Clusters and Favorable Immune Phenotypes in Breast Cancer of the Young Patientsen_US
dc.typeJournal articleen_US
dc.typePeer revieweden_US
dc.description.versionpublishedVersionen_US
dc.rights.holderCopyright 2024 the authorsen_US
dc.source.articlenumber100529en_US
cristin.ispublishedtrue
cristin.fulltextoriginal
cristin.qualitycode2
dc.identifier.doi10.1016/j.modpat.2024.100529
dc.identifier.cristin2279183
dc.source.journalModern Pathologyen_US
dc.identifier.citationModern Pathology. 2024, 37 (8), 100529.en_US
dc.source.volume37en_US
dc.source.issue8en_US


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Navngivelse 4.0 Internasjonal
Except where otherwise noted, this item's license is described as Navngivelse 4.0 Internasjonal