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Annals of Oncology 10:S9-S11, 1999
© 1999 European Society for Medical Oncology

Review

Pathology of incipient pancreatic cancer

R. H. Hruban1,2, R.E. Wilentz1, M. Goggins2, G.J.A. Offerhaus3, C.J. Yeo2,4 and S.E. Kern1,2

1 Department of Pathology, The Johns Hopkins Medical Institutions Baltimore, MD, USA
2 Department of Oncology, The Johns Hopkins Medical Institutions Baltimore, MD, USA
3 Department of Surgery, The Johns Hopkins Medical Institutions Baltimore, MD, USA
4 The Department of Pathology, the Academic Medical Center Amsterdam, The Netherlands

Correspondence to: Ralph H. Hruban, M.D., Meyer 7-181, Department of Pathology, The Johns Hopkins Hospital, 600 N. Wolfe St., Baltimore, MD 21287, USA

Background: An understanding of incipient pancreatic neoplasia is an essential foundation for the future development of effective screening tests for pancreatic cancer. Only when we understand early pancreatic neoplasms will we be able to detect tumors that are curable with surgical resection.

Method: Two approaches have helped define incipient pancreatic neoplasia. First, the histologic examination of pancreata has helped identify the most common histologic lesions in pancreatic tissues adjacent to infiltrating carcinomas. The assumption is that some of these lesions represent the precursors to the infiltrating cancers. Second, advances in molecular genetics now make it possible to define the genetic alterations present in small lesions. The demonstration that a suspected precursor lesion and an infiltrating pancreatic carcinoma share the same genetic alterations would help establish that the lesion is indeed a precursor to infiltrating pancreatic carcinoma.

Results: A spectrum of intraductal proliferations in the pancreas has been found associated with infiltrating adenocarcinoma of the pancreas. These lesions, called "duct lesions," have even been identified in pancreata years before patients develop infiltrating carcinoma. Molecular genetic analysis of these lesions has revealed that they frequently harbor many of the same alterations present in infiltrating carcinoma of the pancreas. These alterations include activation of K-ras and inactivation of p16, p53 and, rarely BRCA2.

Conclusions: From these morphologic and molecular observations, we can now develop a progression model for the development of infiltrating carcinoma of the pancreas. Infiltrating carcinomas of the pancreas may arise from pancreatic duct lesions, and the progression of duct lesions to infiltrating cancer is associated with the accumulation of generalized and specific genetic alterations.

duct lesions, hyperplasia, K-ras, p16, p53, pancreas, pancreas cancer


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