Variation in Precursor Lesions of Pancreatic Cancer Among High-risk Groups

Overview

Journal Clin Cancer Res

Specialty Oncology

Date 2012 Nov 23

PMID 23172884

Citations 31

Authors

Thomas P Potjer

Ingrid Schot

Peter Langer

Johannes T Heverhagen

Martin N J M Wasser

Emily P Slater

Gunter Kloppel

Hans M Morreau

Bert A Bonsing

Wouter H de Vos Tot Nederveen Cappel

Mathias Bargello

Thomas M Gress

Hans F A Vasen

Detlef K Bartsch

Affiliations

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Abstract

Purpose: Pancreatic ductal adenocarcinoma (PDAC) surveillance programs are currently offered to high-risk individuals aiming to detect precursor lesions or PDAC at an early stage. We assessed differences in frequency and behavior of precursor lesions and PDAC between two high-risk groups.

Experimental Design: Individuals with a p16-Leiden germline mutation (N = 116; median age 54 years) and individuals from familial pancreatic cancer (FPC) families (N = 125; median age 47 years) were offered annual surveillance by MRI and magnetic resonance cholangiopancreatography (MRCP) with or without endoscopic ultrasound (EUS) for a median surveillance period of 34 months (0-127 months) or 36 months (0-110 months), respectively. Detailed information was collected on pancreatic cystic lesions detected on MRCP and precursor lesions in surgical specimens of patients who underwent pancreatic surgery.

Results: Cystic lesions were more common in the FPC cohort (42% vs. 16% in p16-Leiden cohort), whereas PDAC was more common in the p16-Leiden cohort (7% vs. 0.8% in FPC cohort). Intraductal papillary mucinous neoplasm (IPMN) was a common finding in surgical specimens of FPC-individuals, and was only found in two patients of the p16-Leiden cohort. In the p16-Leiden cohort, a substantial proportion of cystic lesions showed growth or malignant transformation during follow-up, whereas in FPC individuals most cystic lesions remain stable.

Conclusion: In p16-Leiden mutation carriers, cystic lesions have a higher malignant potential than in FPC-individuals. On the basis of these findings, a more intensive surveillance program may be considered in this high-risk group.

Citing Articles

Surgical aspects related to hereditary pancreatic cancer.

Maurer E, Bartsch D Fam Cancer. 2024; 23(3):341-350.

PMID: 38662263 PMC: 11254980. DOI: 10.1007/s10689-024-00384-1.

Aspects and outcomes of surveillance for individuals at high-risk of pancreatic cancer.

Bogdanski A, van Hooft J, Boekestijn B, Bonsing B, Wasser M, Klatte D Fam Cancer. 2024; 23(3):323-339.

PMID: 38619782 PMC: 11255004. DOI: 10.1007/s10689-024-00368-1.

The role of endoscopic ultrasound in the detection of pancreatic lesions in high-risk individuals.

Overbeek K, Cahen D, Bruno M Fam Cancer. 2024; 23(3):279-293.

PMID: 38573399 PMC: 11255057. DOI: 10.1007/s10689-024-00380-5.

Precursor lesions in familial and hereditary pancreatic cancer.

Pfluger M, Brosens L, Hruban R Fam Cancer. 2024; 23(3):267-278.

PMID: 38319536 DOI: 10.1007/s10689-024-00359-2.

Role of EUS combined with a newly modified scoring system to detect pancreatic high-grade precancerous lesions.

Sagami R, Hayasaka K, Ujihara T, Iwaki T, Katsuyama Y, Harada H Endosc Ultrasound. 2023; 12(1):111-119.

PMID: 36861510 PMC: 10134925. DOI: 10.4103/EUS-D-21-00187.