Please use this identifier to cite or link to this item: https://doi.org/10.1038/s41525-018-0058-3
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dc.titleRecurrent loss of heterozygosity correlates with clinical outcome in pancreatic neuroendocrine cancer
dc.contributor.authorLawrence, B
dc.contributor.authorBlenkiron, C
dc.contributor.authorParker, K
dc.date.accessioned2020-10-20T03:26:12Z
dc.date.available2020-10-20T03:26:12Z
dc.date.issued2018
dc.identifier.citationLawrence, B, Blenkiron, C, Parker, K (2018). Recurrent loss of heterozygosity correlates with clinical outcome in pancreatic neuroendocrine cancer. npj Genomic Medicine 3 (1) : 18. ScholarBank@NUS Repository. https://doi.org/10.1038/s41525-018-0058-3
dc.identifier.issn20567944
dc.identifier.urihttps://scholarbank.nus.edu.sg/handle/10635/177814
dc.description.abstractPancreatic neuroendocrine tumors (pNETs) are uncommon cancers arising from pancreatic islet cells. Here we report the analysis of gene mutation, copy number, and RNA expression of 57 sporadic well-differentiated pNETs. pNET genomes are dominated by aneuploidy, leading to concordant changes in RNA expression at the level of whole chromosomes and chromosome segments. We observed two distinct patterns of somatic pNET aneuploidy that are associated with tumor pathology and patient prognosis. Approximately 26% of the patients in this series had pNETs with genomes characterized by recurrent loss of heterozygosity (LoH) of 10 specific chromosomes, accompanied by bi-allelic MEN1 inactivation and generally poor clinical outcome. Another ~40% of patients had pNETs that lacked this recurrent LoH pattern but had chromosome 11 LoH, bi-allelic MEN1 inactivation, and universally good clinical outcome. The somatic aneuploidy allowed pathogenic germline variants (e.g., ATM) to be expressed unopposed, with RNA expression patterns showing inactivation of downstream tumor suppressor pathways. No prognostic associations were found with tumor morphology, single gene mutation, or expression of RNAs reflecting the activity of immune, differentiation, proliferative or tumor suppressor pathways. In pNETs, single gene mutations appear to be less important than aneuploidy, with MEN1 the only statistically significant recurrently mutated driver gene. In addition, only one pNET in the series had clearly actionable single nucleotide variants (SNVs) (in PTEN and FLCN) confirmed by corroborating RNA expression changes. The two clinically relevant patterns of LoH described here define a novel oncogenic mechanism and a plausible route to genomic precision oncology for this tumor type. © 2018, The Author(s).
dc.rightsAttribution 4.0 International
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.sourceUnpaywall 20201031
dc.subjectBRCA2 protein
dc.subjectCD56 antigen
dc.subjectchromogranin A
dc.subjectcyclin dependent kinase inhibitor 1B
dc.subjectDNA glycosylase MutY
dc.subjectDNA mismatch repair protein MSH2
dc.subjectfibroblast growth factor receptor 3
dc.subjectJanus kinase 2
dc.subjectmessenger RNA
dc.subjectphosphatidylinositol 3,4,5 trisphosphate 3 phosphatase
dc.subjectRNA
dc.subjectsynaptophysin
dc.subjectvon Hippel Lindau protein
dc.subjectaneuploidy
dc.subjectArticle
dc.subjectcancer prognosis
dc.subjectcancer susceptibility
dc.subjectcarcinogenesis
dc.subjectcell differentiation
dc.subjectchromosome 11
dc.subjectclinical outcome
dc.subjectdisease severity
dc.subjectflcn gene
dc.subjectgene
dc.subjectgene expression
dc.subjectgene mutation
dc.subjectgenetic variability
dc.subjectheterozygosity loss
dc.subjecthuman
dc.subjecthuman tissue
dc.subjectmajor clinical study
dc.subjectmen1 gene
dc.subjectmicroarray analysis
dc.subjectNew Zealand
dc.subjectpancreas islet cell tumor
dc.subjectpriority journal
dc.subjectprogression free survival
dc.subjectRNA methylation
dc.subjectsingle nucleotide polymorphism
dc.subjectwhole genome sequencing
dc.typeArticle
dc.contributor.departmentSURGERY
dc.description.doi10.1038/s41525-018-0058-3
dc.description.sourcetitlenpj Genomic Medicine
dc.description.volume3
dc.description.issue1
dc.description.page18
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