Recurrent loss of heterozygosity correlates with clinical outcome in pancreatic neuroendocrine cancer

Lawrence, Ben; Blenkiron, Cherie; Parker, Kate; Tsai, Peter; Fitzgerald, Sandra; Shields, Paula; Robb, Tamsin J.; Yeong, Mee Ling; Krämer, Nicole; James, S.; Black, Michael A.; Fan, Vicky; Poonawala, Nooriyah; Yap, Patrick; Coats, Esther; Woodhouse, Braden J.; Ramsaroop, Reena; Yozu, Masato; Robinson, Bridget A.; Henare, Kimiora; Koea, Jonathan; Johnston, Peter; Carroll, Richard; Connor, Saxon; Morrin, Helen; Elston, Marianne S.; Jackson, Christopher; Reid, Papaarangi; Windsor, John A.; MacCormick, Andrew; Babor, Richard; Bartlett, Adam; Damianovich, Dragan; Knowlton, Nicholas; Grimmond, Sean M.; Findlay, Michael; Print, Cristin G.

doi:10.1038/s41525-018-0058-3

Cited by 41 publications

(51 citation statements)

References 61 publications

(64 reference statements)

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“…However, in this study series, G2 tumours (coinciding with the RPCL cluster) harbouring mutations in DAXX/ATRX and correlating with mutations in mTOR genes were associated with poor prognosis. Another recent targeted/whole-genome sequencing study reported three CN-based clusters (Lawrence et al 2018) similar to those identified in the Scarpa study. Correlation with clinical data demonstrated that tumours in cluster 1 had the poorest prognosis, cluster 2 tumours had more favourable clinical/pathological outcomes, while those in cluster 3 had variable clinical outcomes.…”

Section: Integrated Multi-omic Data Approachessupporting

confidence: 64%

“…However, their penetrance among PanNET cases is currently unknown and warrants further investigation possibly within a clinical genetic referral context. This list has recently been expanded through the identification of novel non-synonymous germline mutations in PIF1 (n = 2), involved in transcriptional regulation and chromatin remodelling, MAPKBP1 (n = 1), a member of the MAPK/ERK signalling pathway (Vandamme et al 2019) known to be co-activated with the PI3K/Akt/mTOR pathway in neuroendocrine tumours through PI3K (Carracedo et al 2008), and identification of a pathogenic germline variant leading to somatic loss of ATM (Lawrence et al 2018).…”

Section: Novel Findingsmentioning

confidence: 99%

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The evolving (epi)genetic landscape of pancreatic neuroendocrine tumours

Pipinikas

Berner

Sposito

et al. 2019

Endocrine-Related Cancer

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Neuroendocrine neoplasms (NENs) are a relatively rare group of heterogeneous tumours originating from neuroendocrine cells found throughout the body. Pancreatic NENs (PanNENs) are the second most common pancreatic malignancy accounting for 1–3% of all neoplasms developing in the pancreas. Despite having a low background mutation rate, driver mutations in MEN1, DAXX/ATRX and mTOR pathway genes (PTEN, TSC1/2) are implicated in disease development and progression. Their increased incidence coupled with advances in sequencing technologies has reignited the interest in PanNEN research and has accelerated the acquisition of molecular data. Studies utilising such technological advances have further enriched our knowledge of PanNENs’ biology through novel findings, including higher-than-expected presence of germline mutations in 17% of sporadic tumours of no familial background, identification of novel mutational signatures and complex chromosomal rearrangements and a dysregulated epigenetic machinery. Integrated genomic studies have progressed the field by identifying the synergistic action between different molecular mechanisms, while holding the promise for deciphering disease heterogeneity. Although our understanding is far from being complete, these novel findings have provided the optimism of shaping the future of PanNEN research, ultimately leading to an era of precision medicine for NETs. Here, we recapitulate the existing knowledge on pancreatic neuroendocrine tumours (PanNETs) and discuss how recent, novel findings have furthered our understanding of these complex tumours.

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Section: Integrated Multi-omic Data Approachessupporting

confidence: 64%

Section: Novel Findingsmentioning

confidence: 99%

The evolving (epi)genetic landscape of pancreatic neuroendocrine tumours

Pipinikas

Berner

Sposito

et al. 2019

Endocrine-Related Cancer

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“…The cohort includes tumors of grades NET G1 (27) and NET G2 (25) NET G3 (4), and NEC (3), 45 samples were primary PanNENs and 14 were metastases (8 liver, 6 lymph nodes). As healthy control we used matched adjacent healthy (24) or distant healthy tissue (27) or blood (4) from the same patient.…”

Section: Sample Characteristicsmentioning

confidence: 99%

“…In addition to driver mutations affecting individual genes, copy number aberrations (CNA) have been used to characterize these tumors 16,[24][25][26] . Recent work has revealed four distinct subtypes based on chromosome arm length CNA patterns: i) recurring copy number losses of specific chromosomes, ii) limited copy number events with mostly loss of chromosome 11, iii) polyploidy tumors and iv) aneuploidy tumors 16 .…”

Section: Introductionmentioning

confidence: 99%

“…Recent work has revealed four distinct subtypes based on chromosome arm length CNA patterns: i) recurring copy number losses of specific chromosomes, ii) limited copy number events with mostly loss of chromosome 11, iii) polyploidy tumors and iv) aneuploidy tumors 16 . In addition, the first two groups harbor MEN1 mutations in combination with loss of chromosome 11, resulting in a bi-allelic inactivation of this tumor suppressor gene 24 . The aneuploid tumors also show frequent DAXX/ATRX loss of expression along with an alternative telomerase lengthening phenotype 25 .…”

Section: Introductionmentioning

confidence: 99%

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DNA methylation reveals distinct cells of origin for pancreatic neuroendocrine carcinomas (PanNECs) and pancreatic neuroendocrine tumors (PanNETs)

Simon

Riemer

Detjen

et al. 2020

Preprint

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Pancreatic Neuroendocrine Neoplasms (PanNENs) comprise a rare and heterogeneous group of tumors derived from neuroendocrine cells of the pancreas. Despite recent genetic and epigenetic characterization, biomarkers for improved patient stratification and personalized therapy are sparse and targeted therapies, including the mTOR inhibitor Everolimus, have shown limited success. To better define PanNENs tumors we performed multi-omic analyses on 59 tumors with varying grades (NET G1, NET G2, NET G3 and NEC), combining mutational profiling with epigenetic analysis and targeted proteomics. An unsupervised approach using DNA methylation profiles uncovered two major subgroups in PanNENs resembling α-like and β-like cells. DNA copy number analysis further divided the α-like subgroup into two distinct groups, indicating differential mechanisms of tumorigenesis from α-cells. β-like tumors however showed two distinct groups at the epigenetic level and suggest NET G3/NEC samples are of β-cell origin.DNA mutation profiling clearly separated α and β-cell derived PanNENs, whereby only αlike tumors had mutations within MEN1/DAXX/ATRX tumor suppressor genes. Targeted proteomic analysis further indicated overexpression of distinct components of the mTOR pathway. Our data provide further insights into the potential mechanisms behind PanNEN heterogeneity and form a basis for future diagnostic and therapy relevant patient stratification.

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