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Kras mutation rate precisely orchestrates ductal derived pancreatic intraepithelial neoplasia and pancreatic cancer

by Thosani, Nirav , Cash, Brooks D. , Younes, Mamoun , Chang, Jeffrey T. , Bailey-Lundberg, Jennifer M. , Pruski, Melissa , Maitra, Anirban , McAllister, Florencia , Bland, Rachael , Guha, Sushovan , Logsdon, Craig D. , Singh, Kanchan

in 13/1 / 13/51 / 631/67/70 / 631/80/304 / 64/110 / 64/60 / 82/79 / 96/106 / 96/63 / Adenocarcinoma / AKT protein / Animal models / Animals / Body weight / Cancer / Carcinoma, Pancreatic Ductal - genetics / Carcinoma, Pancreatic Ductal - metabolism / Carcinoma, Pancreatic Ductal - pathology / Disease Models, Animal / Ectopic expression / Gene Expression Regulation, Neoplastic / Hypotheses / Invasiveness / K-Ras protein / Laboratory Medicine / MAP kinase / Medicine / Medicine & Public Health / Mice / Mice, Transgenic / Mutants / Mutation / Mutation Rate / Mutation rates / p53 Protein / Pancreatic cancer / Pancreatic Ducts - cytology / Pancreatic Ducts - metabolism / Pancreatic Ducts - pathology / Pancreatic Neoplasms - genetics / Pancreatic Neoplasms - metabolism / Pancreatic Neoplasms - pathology / Pathology / Precancerous Conditions - genetics / Precancerous Conditions - metabolism / Precancerous Conditions - pathology / Proteomics / Proto-Oncogene Proteins p21(ras) - genetics / Proto-Oncogene Proteins p21(ras) - metabolism / PTEN protein / Recombination / Recombination, Genetic / Tamoxifen / Trinucleotide repeats / Tumor suppressor genes / Tumors

2021

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Kras mutation rate precisely orchestrates ductal derived pancreatic intraepithelial neoplasia and pancreatic cancer

2021

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Kras mutation rate precisely orchestrates ductal derived pancreatic intraepithelial neoplasia and pancreatic cancer

2021

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Journal Article

Kras mutation rate precisely orchestrates ductal derived pancreatic intraepithelial neoplasia and pancreatic cancer

Thosani, Nirav,

Cash, Brooks D.,

Younes, Mamoun,

Chang, Jeffrey T.,

Bailey-Lundberg, Jennifer M.,

Pruski, Melissa,

Maitra, Anirban,

McAllister, Florencia,

Bland, Rachael,

Guha, Sushovan,

Logsdon, Craig D.,

Singh, Kanchan

2021

Overview

Pancreatic ductal adenocarcinoma (PDAC) is the third leading cause of cancer-related death in the United States. Despite the high prevalence of Kras mutations in pancreatic cancer patients, murine models expressing the oncogenic mutant Kras (Krasmut) in mature pancreatic cells develop PDAC at a low frequency. Independent of cell of origin, a second genetic hit (loss of tumor suppressor TP53 or PTEN) is important for development of PDAC in mice. We hypothesized ectopic expression and elevated levels of oncogenic mutant Kras would promote PanIN arising in pancreatic ducts. To test our hypothesis, the significance of elevating levels of K-Ras and Ras activity has been explored by expression of a CAG driven LGSL-KrasG12V allele (cKras) in pancreatic ducts, which promotes ectopic Kras expression. We predicted expression of cKras in pancreatic ducts would generate neoplasia and PDAC. To test our hypothesis, we employed tamoxifen dependent CreERT2 mediated recombination. Hnf1b:CreERT2;KrasG12V (cKrasHnf1b/+) mice received 1 (Low), 5 (Mod) or 10 (High) mg per 20 g body weight to recombine cKras in low (cKrasLow), moderate (cKrasMod), and high (cKrasHigh) percentages of pancreatic ducts. Our histologic analysis revealed poorly differentiated aggressive tumors in cKrasHigh mice. cKrasMod mice had grades of Pancreatic Intraepithelial Neoplasia (PanIN), recapitulating early and advanced PanIN observed in human PDAC. Proteomics analysis revealed significant differences in PTEN/AKT and MAPK pathways between wild type, cKrasLow, cKrasMod, and cKrasHigh mice. In conclusion, in this study, we provide evidence that ectopic expression of oncogenic mutant K-Ras in pancreatic ducts generates early and late PanIN as well as PDAC. This Ras rheostat model provides evidence that AKT signaling is an important early driver of invasive ductal derived PDAC. In this study, the authors provide evidence that ectopic expression of oncogenic mutant Kras in pancreatic ducts generates early and late (PanIN) and pancreatic ductal adenocarcinoma (PDAC) . They characterized this Ras rheostat model which reveals elevated Kras mutation frequency and loss of PTEN are important drivers of PanIN and invasive ductal derived PDAC.

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Publisher

Elsevier Inc,Nature Publishing Group US,Nature Publishing Group

Subject

13/1

/ 13/51

/ 631/67/70

/ 631/80/304

/ 64/110

/ 64/60

/ 82/79