Statewide Retrospective Review of Familial Pancreatic Cancer in Delaware, and Frequency of Genetic Mutations in Pancreatic Cancer Kindreds
Background Considering the typical rapid progression and high mortality of pancreatic cancer (PC), early detection may lead to an improved outcome. To date, there is no safe, sensitive, and cost-effective screening strategy to detect PC. Currently, screening is focused on individuals at the highest...
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Veröffentlicht in: | Annals of surgical oncology 2016-05, Vol.23 (5), p.1729-1735 |
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Sprache: | eng |
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Zusammenfassung: | Background
Considering the typical rapid progression and high mortality of pancreatic cancer (PC), early detection may lead to an improved outcome. To date, there is no safe, sensitive, and cost-effective screening strategy to detect PC. Currently, screening is focused on individuals at the highest risk of developing PC based on family history. A high-risk individual is defined as having two or more first-degree relatives with PC, or one first- or second-degree relative with PC with a confirmed mutation in a gene associated with PC. The
BRCA2
gene is one of the most common genes linked to pancreatic-only cancer families; however, other hereditary cancer syndromes have also been associated with an increased risk for PC.
Methods
We conducted a retrospective review of pedigrees of families with a pancreatic adenocarcinoma cancer diagnosis held in the statewide Ruth Ann Minner High Risk Family Cancer Registry at the Helen F. Graham Cancer Center and Research Institute, Christiana Care Health System, Newark, DE, USA, from 2002 to 2013. The registry was queried based on how many first-, second-, or third-degree relatives of the proband were affected with PC, genetic testing status, and (if applicable) the results. These data were then categorized into families that meet familial PC (FPC) criteria, defined as two first-degree relatives with PC (FPC families), families that did not meet the FPC definition but had one first-degree relative affected with PC (first-degree families), and probands with PC (probands). Each family was counted only once in the analysis, even if multiple family members were tested.
Results
Our analysis revealed that 175 of 597 families fitting any of the above criteria completed genetic testing. Of this cohort, 52 had pathogenic alterations with nine different genes implicated. Overall, 164 of the 175 families that fitted into any of the three categories previously identified had
BRCA1
or
BRCA2 t
esting, either by DNA sequencing or next-generation sequencing via a panel test that included
BRCA1/2
.
BRCA1
pathogenic alterations were noted in 17/164 (10.4 %) and
BRCA2
pathogenic alterations were noted in 23/164 (14.0 %).
FPC families (n
=
46)
42/46 of the FPC families underwent
BRCA1/2
testing, and 11/42 (26 % [95 % CI 12.89–39.49]) had pathogenic alterations. Specifically, 4/42 =
BRCA1
(9.5 %) and 7/42 =
BRCA2
(16.7 %). Additionally, 16/46 of the FPC families underwent exclusively Lynch syndrome (LS) testing, and pathogenic mutations in |
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ISSN: | 1068-9265 1534-4681 |
DOI: | 10.1245/s10434-015-5026-x |