Sara Welinsky scite author profile

Pancreatic cancer (PC) is the third most common cause of cancer-related death in the United States and the 12th most common worldwide. Mortality is high, largely due to late stage of presentation and suboptimal treatment regimens. Approximately 10% of PC cases have a familial basis. The major genetic defect has yet to be identified but may be inherited by an autosomal dominant pattern with reduced penetrance. Several known hereditary syndromes or genes are associated with an increased risk of developing PC and account for approximately 2% of PCs. These syndromes include the hereditary breast-ovarian cancer syndrome, Peutz-Jeghers syndrome, familial atypical multiple mole melanoma, Lynch syndrome, familial polyposis, ataxia-telangiectasia, and hereditary pancreatitis. Appropriate screening using methods such as biomarkers or imaging, with endoscopic ultrasound and magnetic resonance imaging, may assist in the early detection of neoplastic lesions in the high-risk population. If these lesions are detected and treated before the development of invasive carcinoma, PC disease morbidity and mortality may be improved. This review will focus on familial PC and other hereditary syndromes implicated in the increased risk of PC; it will also highlight current screening methods and the future of new screening modalities.

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The Increasing Prevalence of Inflammatory Bowel Diseases Among Jewish Adolescents and the Sociodemographic Factors Associated with Diagnosis

Levi

Shamiss

Fraser

et al. 2013

Inflammatory Bowel Diseases

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Su1066 Quality Indicators for Colonoscopy and the Risk of Interval Cancer in Symptomatic and High Risk Population Treated in an Academic Tertiary Referral Center

Belfer¹,

Geller²,

Vilkin³

et al. 2013

Gastroenterology

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Genetic Variants in Patients With a Family History of Pancreatic Cancer

Zhu

Welinsky

Soper³

et al. 2021

Pancreas

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Objectives: Up to 15% of pancreatic cancer is hereditary. We aim to study the prevalence of pathogenic germline variants (PGVs) in patients referred for genetic counseling with a family history (FH) of pancreatic cancer. Methods:We performed a retrospective single institution cohort study of individuals who underwent cancer genetic counseling with a FH of pancreatic cancer. Results:We identified 314 patients. Genetic testing was performed in 291 (92.7%) and 187 (59.6%) underwent expanded multigene panel testing. Fifty-four PGVs were found in 53 (16.9%) individuals; PGVs in BRCA1/2 (37%) were most common. Seventy-two variants of uncertain significance (VUS) were found in 58 (18.5%) individuals; VUS in ATM (16.7%) were the most common. Of the 112 (35.4%) with a first-degree family member with pancreatic cancer, 14 PGVs were identified in 14 (12.5%) individuals and 28 VUS were identified in 21 (18.8%) individuals. After genetic testing, 47 (15.0%) individuals met International Cancer of the Pancreas Screening criteria and 67 (21.3%) met American College of Gastroenterology criteria for pancreatic surveillance.Conclusions: Genetic testing of individuals with a FH of pancreatic cancer represents an opportunity to identify individuals who may be candidates for pancreatic surveillance.

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Sara Welinsky

How reliable is immunohistochemical staining for DNA mismatch repair proteins performed after neoadjuvant chemoradiation?

Familial Pancreatic Cancer and the Future of Directed Screening

The Increasing Prevalence of Inflammatory Bowel Diseases Among Jewish Adolescents and the Sociodemographic Factors Associated with Diagnosis

Su1066 Quality Indicators for Colonoscopy and the Risk of Interval Cancer in Symptomatic and High Risk Population Treated in an Academic Tertiary Referral Center

Genetic Variants in Patients With a Family History of Pancreatic Cancer

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