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Phenotypic expression in familial adenomatous polyposis: partial prediction by mutation analysis

Phenotypic expression in familial adenomatous polyposis: partial prediction by mutation analysis
Phenotypic expression in familial adenomatous polyposis: partial prediction by mutation analysis

The phenotypic expression in familial adenomatous polyposis (FAP) is variable. This study compares the phenotype of 27 patients with an identical 5 base pair (bp) deletion at codon 1309 with a group of 61 matched patients with FAP where knowledge of specific mutations is not available and with seven other different mutations in 24 subjects. Patients with the codon 1309 deletion have significantly more colorectal polyps at the time of colectomy than age and sex matched FAP controls (p = 0.0001). The median number of polyps in colectomy specimens of patients with the deletion at condon 1309 was 4000 (interquartile (IQ) range 3000-4875), compared with 600 (IQ range 488-1400) in the matched controls. Mutations at codon 1323, 1407, and 233 were also associated with large numbers of polyps. Desmoid disease and extracolonic cancers were more common with the mutation at codon 1309 (p = 0.003). In conclusion, there may be a correlation between a specific germline mutation and the number of large bowel polyps. There is residual heterogeneity in phenotypic expression, however, and this may result from the influence of other genes, specific environmental factors or chance.

0017-5749
1622-1623
Nugent, K. P.
79fcb89d-6ff2-47b8-ac2c-2afb24954456
Phillips, R. K.S.
d23a75c7-986b-4a83-87e4-e22abae5ade2
Hodgson, S. V.
a425a93c-a1b2-4198-b2ff-53ca1cb0af9c
Cottrell, S.
dcab0a95-33e1-4fd3-af10-bbdf04e0eb7a
Smith-Ravin, J.
58abc12a-8bb6-47ca-b965-5704cee5d52d
Pack, K.
00558f1f-b79a-421e-8b18-c69524396c61
Bodmer, W. F.
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Nugent, K. P.
79fcb89d-6ff2-47b8-ac2c-2afb24954456
Phillips, R. K.S.
d23a75c7-986b-4a83-87e4-e22abae5ade2
Hodgson, S. V.
a425a93c-a1b2-4198-b2ff-53ca1cb0af9c
Cottrell, S.
dcab0a95-33e1-4fd3-af10-bbdf04e0eb7a
Smith-Ravin, J.
58abc12a-8bb6-47ca-b965-5704cee5d52d
Pack, K.
00558f1f-b79a-421e-8b18-c69524396c61
Bodmer, W. F.
2fc548b6-4ed6-416b-aeda-fcdaa7ebfaa1

Nugent, K. P., Phillips, R. K.S., Hodgson, S. V., Cottrell, S., Smith-Ravin, J., Pack, K. and Bodmer, W. F. (1994) Phenotypic expression in familial adenomatous polyposis: partial prediction by mutation analysis. Gut, 35 (11), 1622-1623. (doi:10.1136/gut.35.11.1622).

Record type: Article

Abstract

The phenotypic expression in familial adenomatous polyposis (FAP) is variable. This study compares the phenotype of 27 patients with an identical 5 base pair (bp) deletion at codon 1309 with a group of 61 matched patients with FAP where knowledge of specific mutations is not available and with seven other different mutations in 24 subjects. Patients with the codon 1309 deletion have significantly more colorectal polyps at the time of colectomy than age and sex matched FAP controls (p = 0.0001). The median number of polyps in colectomy specimens of patients with the deletion at condon 1309 was 4000 (interquartile (IQ) range 3000-4875), compared with 600 (IQ range 488-1400) in the matched controls. Mutations at codon 1323, 1407, and 233 were also associated with large numbers of polyps. Desmoid disease and extracolonic cancers were more common with the mutation at codon 1309 (p = 0.003). In conclusion, there may be a correlation between a specific germline mutation and the number of large bowel polyps. There is residual heterogeneity in phenotypic expression, however, and this may result from the influence of other genes, specific environmental factors or chance.

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Published date: November 1994

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Local EPrints ID: 445569
URI: http://eprints.soton.ac.uk/id/eprint/445569
ISSN: 0017-5749
PURE UUID: 5c6d4321-3a05-4424-9237-17f2a6c21a40

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Date deposited: 16 Dec 2020 17:31
Last modified: 16 Mar 2024 09:43

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Contributors

Author: K. P. Nugent
Author: R. K.S. Phillips
Author: S. V. Hodgson
Author: S. Cottrell
Author: J. Smith-Ravin
Author: K. Pack
Author: W. F. Bodmer

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