Analysis of K- ras oncogene mutations in chronic pancreatitis with ductal hyperplasia

Background. K-ras oncogene mutations have been identified in up to 95% of pancreatic cancers, implying their critical role in their molecular pathogenesis. However, the earliest stage in which K-ras mutations can be detected in potential precursor lesions of pancreatic cancer remains unclear. This s...

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Bibliographic Details
Published in:Surgery 1997, Vol.121 (1), p.42-49
Main Authors: Rivera, Jaime A, Rall, Christopher J.N, Graeme-Cook, Fiona, Castillo, Carlos Fernández-del, Shu, Pei, Lakey, Nathan, Tepper, Robert, Rattner, David W, Warshaw, Andrew L, Rustgi, Anil K
Format: Article
Language:English
Subjects:
Adult
Aged
Base Sequence
Biological and medical sciences
Chronic Disease
DNA - genetics
Female
Gastroenterology. Liver. Pancreas. Abdomen
Genes, ras
Humans
Hyperplasia
Liver. Biliary tract. Portal circulation. Exocrine pancreas
Male
Medical sciences
Middle Aged
Mutation
Nucleic Acid Hybridization
Oligonucleotide Probes
Other diseases. Semiology
Pancreatic Ducts - pathology
Pancreatitis - genetics
Pancreatitis - pathology
Polymerase Chain Reaction
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Summary:Background. K-ras oncogene mutations have been identified in up to 95% of pancreatic cancers, implying their critical role in their molecular pathogenesis. However, the earliest stage in which K-ras mutations can be detected in potential precursor lesions of pancreatic cancer remains unclear. This study evaluates pancreatic ductal hyperplasia in the setting of chronic pancreatitis, which predisposes to pancreatic cancer development, for K-ras codon 12 and 13 mutations. Methods. Paraffin-embedded surgical specimens from 42 patients with chronic pancreatitis were examined microscopically for the presence of ductal hyperplasia. Both hyperplastic and nonhyperplastic ducts were microdissected from the specimens that contained hyperplasia (11 of 42). Four of the remaining specimens without hyperplasia served as controls. Genomic DNA was extracted, and polymerase chain reaction and amplification of the K-ras oncogene was performed. Polymerase chain reaction products were evaluated by means of hybridization to mutant specific oligonucleotide probes and by means of automated DNA sequencing. Results. K-ras codon 12 mutations representing glycine to valine substitutions were present in 2 of (18%) 11 patients with ductal hyperplasia. No mutations were found in the controls without ductal hyperplasia. Conclusions. Our study supports the premise that K-ras mutations develop in a subset of chronic pancreatitis associated hyperplasia and provides a genetic basis for the potential progression of chronic pancreatitis to pancreatic cancer.
ISSN:0039-6060
1532-7361
DOI:10.1016/S0039-6060(97)90181-1