Pancreatic cancer genomes reveal aberrations in axon guidance pathway genes

Biankin, Andrew V.; Waddell, Nicola; Kassahn, Karin S.; Gingras, Marie Claude; Muthuswamy, Lakshmi; Johns, Amber; Miller, David; Wilson, Peter J.; Patch, Ann Marie; Wu, Jianmin; Chang, David K.; Cowley, Mark J.; Gardiner, Brooke; Song, Sarah; Harliwong, Ivon; Idrisoglu, Senel; Nourse, Craig; Nourbakhsh, Ehsan; Manning, Suzanne; Wani, Shivangi; Gongora, Milena; Pajic, Marina; Scarlett, Christopher J.; Gill, Anthony J.; Pinho, Andreia V.; Rooman, Ilse; Anderson, Matthew; Holmes, Oliver; Leonard, Conrad; Taylor, Darrin; Wood, Scott; Xu, Qinying; Nones, Kátia; Fink, J. Lynn; Christ, Angelika N.; Bruxner, Timothy J. C.; Cloonan, Nicole; Kolle, Gabriel; Newell, Felicity; Pinese, Mark; Mead, R. Scott; Humphris, Jeremy L.; Kaplan, Warren; Jones, Marc D.; Colvin, Emily K.; Nagrial, Adnan; Humphrey, Emily S.; Chou, Angela; Chin, Venessa T.; Chantrill, Lorraine A.; Mawson, Amanda; Samra, Jaswinder S.; Kench, James G.; Lovell, Jessica A.; Daly, Roger J.; Merrett, Neil D.; Toon, Christopher W.; Epari, Krishna; Nguyen, Nam Q.; Barbour, Andrew P.; Zeps, Nikolajs; Kakkar, Nipun; Zhao, Fengmei; Wu, Yuan; Wang, Min; Muzny, Donna M.; Fisher, William E.; Brunicardi, F. Charles; Hodges, Sally E.; Reid, Jeffrey G.; Drummond, Jennifer; Chang, Kyle; Han, Yi; Lewis, Lora; Dinh, Huyen; Buhay, Christian; Beck, Timothy; Timms, Lee; Sam, Michelle; Begley, Kimberly; Brown, Andrew; Pai, Deepa; Panchal, Ami; Buchner, Nicholas; Borja, Richard de; Denroche, Robert E.; Yung, Christina K.; Serra, Stefano; Onetto, Nicole; Mukhopadhyay, Debabrata; Tsao, Ming‐Sound; Shaw, Patricia; Petersen, Gloria M.; Gallinger, Steven; Hruban, Ralph H.; Maitra, Anirban; Iacobuzio‐Donahue, Christine A.; Schulick, Richard D.; Wolfgang, Christopher L.; Morgan, Richard A.; Lawlor, Rita T.; Capelli, Paola; Corbo, Vincenzo; Scardoni, Maria; Tortora, Giampaolo; Tempero, Margaret A.; Mann, Karen; Jenkins, Nancy A.; Pérez–Mancera, Pedro A.; Adams, David J.; Largaespada, David A.; Wessels, Lodewyk; Rust, Alistair G.; Stein, Lincoln; Tuveson, David A.; Copeland, Neal G.; Musgrove, Elizabeth A.; Scarpa, Aldo; Eshleman, James R.; Hudson, Thomas J.; Sutherland, Robert L.; Wheeler, David A.; Pearson, John V.; Mcpherson, John Douglas; Gibbs, Richard A.; Grimmond, Sean M.

doi:10.1038/nature11547

Cited by 1,750 publications

(1,580 citation statements)

References 41 publications

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“…Prior studies have reported STK11 mutations in a similar percentage of IPMNs (9%) [8]. Prior studies have found ATM and CDH1 somatic mutations in a small percentage of pancreatic ductal adenocarcinomas, but these mutations have not yet been reported in IPMNs [33,34]. Somatic mutations in IDH1, PTEN, FGFR3, NRAS and SRC have not been reported in IPMNs or in pancreatic ductal adenocarcinomas [33,34].…”

Section: Discussionmentioning

confidence: 94%

“…Prior studies have found ATM and CDH1 somatic mutations in a small percentage of pancreatic ductal adenocarcinomas, but these mutations have not yet been reported in IPMNs [33,34]. Somatic mutations in IDH1, PTEN, FGFR3, NRAS and SRC have not been reported in IPMNs or in pancreatic ductal adenocarcinomas [33,34]. CTNNB1 mutations are characteristic of pancreatic solid and pseudopapillary tumours, but nuclear expression of β-catenin has been described in some IPMNs [17].…”

Section: Discussionmentioning

confidence: 99%

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Targeted next-generation sequencing of cancer genes dissects the molecular profiles of intraductal papillary neoplasms of the pancreas.

et al. 2014

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Section: Discussionmentioning

confidence: 94%

Section: Discussionmentioning

confidence: 99%

Targeted next-generation sequencing of cancer genes dissects the molecular profiles of intraductal papillary neoplasms of the pancreas.

et al. 2014

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“…In prostate cancer, targeted next-generation sequencing has revealed an 8% incidence of ATM mutations (59). ATM is also one of the most commonly mutated genes in pancreatic cancer (60) or lung adenocarcinoma (61). In colorectal cancer, loss of ATM protein expression is associated with worse prognosis, based on immunohistochemical analysis of stage II/III cancers (62), and a high percentage of ATM-mutated cases has been reported by COSMIC (47).…”

Section: Somatic Atm Mutations In Cancermentioning

confidence: 99%

ATM Mutations in Cancer: Therapeutic Implications

Choi¹,

Kipps²,

Kurzrock³

2016

Molecular Cancer Therapeutics

360

296

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Activation of checkpoint arrest and homologous DNA repair are necessary for maintenance of genomic integrity during DNA replication. Germ-line mutations of the ataxia telangiectasia mutated (ATM) gene result in the well-characterized ataxia telangiectasia syndrome, which manifests with an increased cancer predisposition, including a 20% to 30% lifetime risk of lymphoid, gastric, breast, central nervous system, skin, and other cancers. Somatic ATM mutations or deletions are commonly found in lymphoid malignancies, as well as a variety of solid tumors. Such mutations may result in chemotherapy resistance and adverse prognosis, but may also be exploited by existing or emerging targeted therapies that produce synthetic lethal states.

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“…However, previously it has been shown that the long-term maintenance in culture of PDAC cell lines, such as BxPC-3, CFPAC-1 and PANC-1 cells 33,34 , resulted in distinct and irreversible loss of crucial genetic and biologic properties. This included the occurrence of distinct stem cell populations and complex genomic aberrations, affecting critical signaling pathways 35,36 . A more recent study used PDAC primary cell cultures obtained from ascites, demonstrating the establishment of cell masses on the CAM that were consistent with the in vitro studies of tumorigenicity of the PDAC primary cultures 37 .…”

Section: Discussionmentioning

confidence: 99%

Development of bioluminescent chick chorioallantoic membrane (CAM) models from primary pancreatic cancer cells: A platform for drug testing

León

Rovithi

Avan³

et al. 2017

Pancreatology

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The aim of the present study was to develop chick-embryo chorioallantoic membrane (CAM) bioluminescent tumor models employing low passage cell cultures obtained from primary pancreatic ductal adenocarcinoma (PDAC) cells. Primary PDAC cells transduced with lentivirus expressingFirefly-luciferase (Fluc) were established and inoculated onto the CAM membrane, with >80% engraftment. Fluc signal reliably correlated with tumor growth. Tumor features were evaluated by immunohistochemistry and genetic analyses, including analysis of mutations and mRNA expression of PDAC pivotal genes, as well as microRNA (miRNA) profiling. These studies showed that CAM tumors had histopathological and genetic characteristic comparable to the original tumors. We subsequently tested the modulation of key miRNAs and the activity of gemcitabine and crizotinib on CAM tumors, showing that combination treatment resulted in 63% inhibition of tumor growth as compared to control (p < 0.01). These results were associated with reduced expression of miR-21 and increased expression of miR-155. Our study provides the first evidence that transduced primary PDAC cells can form tumors on the CAM, retaining several histopathological and (epi)genetic characteristics of original tumors. Moreover, our results support the use of these models for drug testing, providing insights on molecular mechanisms underlying antitumor activity of new drugs/combinations.With less than 7% of patients alive five years after diagnosis, pancreatic ductal adenocarcinoma (PDAC) exhibits one of the poorest prognoses of all solid tumors. Despite extensive clinical efforts, the outcome of this malignancy has not improved in the last decade, and PDAC is expected to become the second deadliest cancer, after lung cancer, by 2030 1,2 .Gaining more insight into the mechanisms that delineate tumor progression in PDAC could ultimately provide more successful therapeutic approaches. To this end, genetically engineered mouse models (GEMMs) have provided a powerful tool, developing tumors that recapitulate both the underlying biology and the dense desmoplastic reaction of PDACs. This stromal reaction has been considered for years as one of the mediators of resistance to chemotherapy 3 . However, experimental and clinical evidence demonstrated that anti-stromal approaches may favour PDAC aggressiveness, reinforcing the need to critically revisit the complexity of cancer-stroma interactions for translational and pharmacological implications 4 . Recent studies suggested that early passages of primary PDAC cells and "avatar" mice can mimic the genetic diversity that characterizes the human disease and might be better predictors of drug activity, including the standard treatment with gemcitabine 5,6 .Despite several studies used such in vivo models in order to promote drug development and selection, their costs and complexity impaired the translation of these results in the clinical setting. Novel, cost-effective models that similarly mimic tumor biology and provide faster information on the activ...

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Pancreatic cancer genomes reveal aberrations in axon guidance pathway genes

Cited by 1,750 publications

References 41 publications

Targeted next-generation sequencing of cancer genes dissects the molecular profiles of intraductal papillary neoplasms of the pancreas.

Targeted next-generation sequencing of cancer genes dissects the molecular profiles of intraductal papillary neoplasms of the pancreas.

ATM Mutations in Cancer: Therapeutic Implications

Development of bioluminescent chick chorioallantoic membrane (CAM) models from primary pancreatic cancer cells: A platform for drug testing

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