Article Text
Abstract
BACKGROUND The phenotypic spectrum of familial adenomatous polyposis (FAP) varies from the classic appearance of hundreds of adenomatous colonic polyps in the young adult and early onset colorectal cancer, to the occurrence of sparse adenomas in the older adult, “attenuated” FAP, due to mutations at the 5′ or 3′ ends of the APC gene.
AIMS To investigate marked intrafamilial phenotypic variation occurring in a family with anAPC gene mutation in exon 9.
PATIENTS An extended kindred of 22 people of whom 16 had colorectal neoplasia and/or wereAPC mutation carriers.
RESULTS Phenotypic manifestation varied from classic FAP to a complete lack of clinical or endoscopic, or bioptic disease in five people in three different generations. This occurred in four of them over two generations, in spite of having a confirmed 11 bp insertion causing a frame shift and stop codon (363) in exon 9 of the APC gene.
CONCLUSIONS At present, it is assumed that in this family there is alternative splicing of theAPC gene, and/or unidentified modifying genetic factors. The family illustrates the importance of genetic testing in evaluating carrier status and not just clinical examination. This clinical observation also high- lights the dilemma in recognising the possible contribution of low penetrance germlineAPC mutations to what has been considered “sporadic” colorectal neoplasia.
- APC gene
- familial adenomatous polyposis
- phenotype variation
- modifying genes
- alternative splicing
Abbreviations used in this paper
- FAP
- familial adenomatous polyposis
- CHRPE
- congenital hypertrophy of the retinal pigment epithelium
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Abbreviations used in this paper
- FAP
- familial adenomatous polyposis
- CHRPE
- congenital hypertrophy of the retinal pigment epithelium