High frequency of Ki-ras codon 12 mutations in pancreatic adenocarcinomas

Tumor grade of differentiation according to Klceppel (1984).-2Tumor grade, classified as suggested by the American Joint Committee (1977) with T (tumor size), N (nodular status), and M (metastasis), see also te~t.-~SubstiNtion of the wild-type (wt) Ki-ras 12 allele coding for glycine by amino acids

## Abstract Mutated __ras__ genes have been found to be conspicuously absent from primary tumors of the esophagus, although high expression of ras p21 oncoprotein in some esophageal squamous cell carcinomas and mutations of the Ki‐ and Ha‐__ras__ genes in esophageal carcinoma cell lines have been r

## Abstract __N__‐Methylnitrosourea (NMU)—induced codon 12 Ki‐__ras__ mutations were analyzed in premalignant thymic lymphomas from C57BL/6J mice by using a selective polymerase chain reaction amplification strategy. The frequency of codon 12 Ki‐__ras__ mutations was 67% (16 of 24) in NMU‐treated a

## Abstract We have used the polymerase chain reaction and dideoxynucleotide sequencing to amplify and sequence exons 1 and 2 of the c‐Ki‐__ras__ proto‐oncogene from the normal Syrian golden hamster. Similar methods were employed to screen for the presence of point mutations in the c‐Ki‐__ras__ onc

## Abstract In A/J strain mice, the carcinogen urethan induces lung adenomas and adenocarcinomas that contain Ki‐__ras__‐activating mutations primarily in codon 61. These mutations affect the middle adenine in codon 61 resulting in the substitution of either arginine (AT→GC transition) or leucine (

## Abstract Activation of the c‐Ki‐__ras__ proto‐oncogene is more common in carcinomas of the pancreas than in other human carcinomas. Most such carcinomas are of the ductal cell phenotype. Ductal adenocarcinomas of the hamster pancreas have similar mutations, but acinar cell carcinomas of the mous