Affiliation:
1. Gastroenterology and Hepatology Department Endoscopy Unit Puerta de Hierro University Hospital Madrid Spain
2. Molecular Genetics Unit, Laboratory Medicine Department Puerta de Hierro University Hospital Madrid Spain
3. Hereditary Cancer Unit, Medical Oncology Department Puerta de Hierro University Hospital Madrid Spain
Abstract
AbstractBackgroundJuvenile Polyposis Syndrome (JPS) is a rare autosomal dominant hereditary disorder characterized by the development of multiple hamartomatous gastrointestinal polyps. Here, we present a case of JPS with a mosaic variant in SMAD4.MethodsExome sequencing TRIO analysis, using germline DNA from the biological mother and father along with the index case (IC).ResultsA 46‐year‐old male with no family history of cancer presented with chronic iron deficiency anemia and was diagnosed with massive gastric polyposis (≥100 polyps). At the age of 59, he underwent a total gastrectomy, revealing numerous polyps occupying the entire gastric mucosa, including a 5 cm gastric hyperplastic polyp with high‐grade dysplasia and focal adenocarcinoma. TRIO analysis identified the c.386A>C p.(Asn129Thr) variant in the SMAD4 gene at an allele frequency (AF) of 22%, suggesting its mosaic origin. Subsequently, the variant was found in heterozygosity in the IC's son, who exhibited two subcentimeter polyps in the colon and seven inflammatory gastric polyps with gastric inflammatory areas and hyperplasia, suggesting that the c.386A>C p.(Asn129Thr) variant in SMAD4 segregated with the phenotype.ConclusionOur study provides evidence supporting the classification of the c.386A>C p.(Asn129Thr) variant in SMAD4 as a likely pathogenic variant. This finding contributes to improved accuracy in the diagnosis and genetic counseling of JPS.
Subject
Genetics (clinical),Genetics,Molecular Biology