Multiple primaries in pancreatic cancer patients: indicator of a genetic predisposition?

doi:10.1093/ije/29.6.999

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International Journal of Epidemiology 2000;29:999-1003
© International Epidemiological Association 2000

Multiple primaries in pancreatic cancer patients: indicator of a genetic predisposition?

Berthold Gerdes^a, Andreas Ziegler^b, Annette Ramaswamy^c, Anja Wild^a, Peter Langer^a and Detlef K Bartsch^a

^a Department of General Surgery,
^b Institute of Medical Biometry and Epidemiology and
^c Department of Pathology, Philipps University of Marburg, D-35033 Marburg, Germany.

Reprint requests: Berthold Gerdes, Department of General Surgery, Philipps University of Marburg, Baldingerstraße, 35033 Marburg, Germany. E-mail: Gerdes{at}mailer.uni-marburg.de

Background The genetic basis of several familial cancers includingbreast and colon cancers has been identified recently. The occurrenceof multiple cancers in one individual is also suggestive ofa genetic predisposition. To evaluate inherited predispositionin pancreatic cancer we compared the clinical data of pancreaticcancer patients with and without multiple primaries as wellas the frequency of malignancies among their relatives.

Methods Detailed data on 69 pancreatic cancer patients includedsurvival time and TNM-classification. Index case data were separatedinto two groups. The first group (group 1) developed only pancreaticcancer during their lifetime, whereas the second group (group2) developed additional primary tumours. A systematic familyhistory was taken from 59 of these pancreatic cancer patientsusing a standardized questionnaire. The pancreatic cancers andthe multiple primaries of the 59 patients were histologicallyproven.

Results Of the 69 pancreatic cancer patients, 13 (18.8%) hadmultiple primaries. Neither the clinical data nor the survivaldata of the index cases revealed differences between the twogroups (all nominal P-values >0.05). In the family historystudy blood relatives developed a malignancy in 51% (24 of 47)of the families in group 1 compared to 75% (9 of 12) in group2. The risk of relatives in group 2 of developing a malignanttumour was significantly higher (P = 0.034) than in group 1after adjustments for family size and age of disease onset ofthe index case. The cancer spectrum of the 59 families mainlyincluded tumours of the digestive tract and the reproductiveorgans.

Conclusions A multiple primary cancer history is a common conditionamong pancreatic cancer patients. Relatives of these patientsseem to have an increased risk for the development of distinctmalignant solid tumours, which might be caused by an inheritedpredisposition. Clinical and genetic investigation of pancreaticcancer patients with multiple primaries and their families mightlead to the identification of predisposing gene defects providinga new goal for the understanding of a shared genetic basis ofdifferent solid tumours.

Keywords Multiple primaries, pancreatic carcinoma, family history method, genetics

Accepted 19 April 2000

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