Abstract
Colo-Rectal Cancer is a common cancer worldwide with 5–10% cases being hereditary. Familial Adenomatous Polyposis (FAP) syndrome is due to germline mutations in the APC or rarely MUTYH gene. NTHL1, POLD1, POLE have been recently reported in previously unexplained FAP cases. Unlike the Caucasian population, FAP phenotype and its genotypic associations have not been widely studied in several geoethnic groups. We report the first FAP cohort from South Asia and the only non-Caucasian cohort with comprehensive analysis of APC, MUTYH, NTHL1, POLD1, POLE genes. In this cohort of 112 individuals from 53 FAP families, we detected germline APC mutations in 60 individuals (45 families) and biallelic MUTYH mutations in 4 individuals (2 families). No NTHL1, POLD1, POLE mutations were identified. Fifteen novel APC mutations and a new Indian APC mutational hotspot at codon 935 were identified. Eight very rare FAP phenotype or phenotypes rarely associated with mutations outside specific APC regions were observed. APC genotype-phenotype association studies in different geo-ethnic groups can enrich the existing knowledge about phenotypic consequences of distinct APC mutations and guide counseling and risk management in different populations. A stepwise cost-effective mutation screening approach is proposed for genetic testing of south Asian FAP patients.
Highlights
Familial Adenomatous Polyposis (FAP) is characterized by the early onset of hundreds to thousands of adenomatous polyps throughout the colon and rectum with over 90% risk of development of carcinoma in one or more of the polyps[1]
Our study is the first report of a South Asian cohort of 53 FAP families and the only non-Caucasian FAP cohort analysed for all the 5 adenomatous polyposis associated genes
The high mutation detection rate of 89% in our cohort reflects the appropriateness of our clinical characterization for making the syndromic diagnosis and the comprehensive genetic analysis for APC and MUTYH including Multiplex ligation-dependent probe amplification (MLPA)
Summary
FAP is characterized by the early onset of hundreds to thousands of adenomatous polyps throughout the colon and rectum with over 90% risk of development of carcinoma in one or more of the polyps[1]. Correlation between the location of mutations in APC gene (genotype) and the clinical phenotype in terms of the number of polyps, age of onset of polyps and CRC and distinct extracolonic manifestations is well described[8]. APC genotype-phenotype association studies in different geo-ethnic groups can enrich the existing knowledge about phenotypic consequences of distinct APC mutations and guide counseling and risk management in different populations. This is the first FAP cohort being reported from South Asia and the only non-Caucasian cohort with comprehensive molecular genetic analysis of all the five adenomatous polyposis associated genes (APC, MUTYH, NTHL1, POLD1 and POLE)
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