| Literature DB >> 8957088 |
J Lei1, T T Zou, Y Q Shi, X Zhou, K N Smolinski, J Yin, R F Souza, R Appel, S Wang, K Cymes, O Chan, J M Abraham, N Harpaz, S J Meltzer.
Abstract
Homozygously Deleted in Pancreatic Cancer 4 (DPC4), a recently identified candidate tumor suppressor gene, was previously shown to be altered in human pancreatic cancers. We examined DPC4 mutation in 30 examples of three other types of gastrointestinal malignancy: 10 esophageal cancers, 10 gastric cancers and 10 colorectal cancers occurring in the preneoplastic condition, ulcerative colitis. The entire coding region of DPC4 (including all 11 exons) was analysed by either direct sequencing of PCR product or the in vitro synthesized protein assay. No coding region mutations of DPC4 were found in any of the samples examined. Our results suggest that inactivation of DPC4 may not be important in the majority of these types of gastrointestinal cancer.Entities:
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Year: 1996 PMID: 8957088
Source DB: PubMed Journal: Oncogene ISSN: 0950-9232 Impact factor: 9.867