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Allele-specific genomic data elucidate the role of somatic gain and copy-number neutral loss of heterozygosity in cancer

Yari Ciani, Tarcisio Fedrizzi, Davide Prandi, Francesca Lorenzin, Alessio Locallo, Paola Gasperini, Gian Marco Franceschini, Matteo Benelli, Olivier Elemento, Luca L. Fava, Alberto Inga, Francesca Demichelis

Cell systems(2022)

引用 8|浏览31
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摘要
Pan-cancer studies sketched the genomic landscape of the tumor types spectrum. We delineated the purity and ploidy-adjusted allele-specific profiles of 4,950 patients across 27 tumor types from the Cancer Genome Atlas (TCGA). Leveraging allele-specific data, we reclassified as loss of heterozygosity (LOH) 9% and 7% of apparent copy-number wild-type and gain calls, respectively, and overall observed more than 18 million allelic imbalance somatic events at the gene level. Reclassification of copy-number events revealed associations between driver mutations and LOH, pointing out the timings between the occurrence of point mutations and copy-number events. Integrating allele-specific genomics and matched transcriptomics, we observed that allele-specific gene status is relevant in the regulation of TP53 and its targets. Further, we disclosed the role of copy-neutral LOH in the impairment of tumor suppressor genes and in disease progression. Our results highlight the role of LOH in cancer and contribute to the understanding of tumor progression.
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