Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic
The Cleveland Clinic has followed 1288 patients with inflammatory bowel disease (IBD) (437 with mucosa! ulcerative colitis and 851 with Crohn's disease) from 1955 through 1984. Of the 437 patients with mucosal ulcerative colitis, the index patient had one or more family members develop IBD. The...
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Series: | Canadian Journal of Gastroenterology |
Online Access: | http://dx.doi.org/10.1155/1990/458980 |
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doaj-ac105510c01243858bfb0ad9ef19007f2020-11-24T21:30:39ZengHindawi LimitedCanadian Journal of Gastroenterology0835-79001990-01-014735035410.1155/1990/458980Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland ClinicWM MichenerM CaulfieldRG FarmerR WyllieK CotmanJ HertzerThe Cleveland Clinic has followed 1288 patients with inflammatory bowel disease (IBD) (437 with mucosa! ulcerative colitis and 851 with Crohn's disease) from 1955 through 1984. Of the 437 patients with mucosal ulcerative colitis, the index patient had one or more family members develop IBD. These data indicate the need for the treating physician to institute case-finding questions within the family so that early diagnoses can be established. From 1975 through 1984, 94 patients had a positive family history and 63 had additional family members with disease. The highest risk group was the sibling-sibling group (6.4% in mucosa! ulcerative colitis and 8.3% in Crohn's disease). Both groups had similar percentages for all immediate family members; namely, 16.5% and 17.3%. In the group of patients reported from 1975 to 1984, the location of disease in the index patient and the immediate family member was the same in 67.5% and different in 30.0%. In this same group of patients, the disease similarity in the index patient and the immediate family member was the same in 86.8% and different in 12.0%. These data suggest that while genetic factors undoubtedly increase the susceptibility for IBD, there is no specific genetic pattern identified. Also, environmental and other factors may be present. The data also suggest that the age of onset is a factor, perhaps showing increased association with a positive family history.http://dx.doi.org/10.1155/1990/458980 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
WM Michener M Caulfield RG Farmer R Wyllie K Cotman J Hertzer |
spellingShingle |
WM Michener M Caulfield RG Farmer R Wyllie K Cotman J Hertzer Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic Canadian Journal of Gastroenterology |
author_facet |
WM Michener M Caulfield RG Farmer R Wyllie K Cotman J Hertzer |
author_sort |
WM Michener |
title |
Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic |
title_short |
Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic |
title_full |
Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic |
title_fullStr |
Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic |
title_full_unstemmed |
Genetic Counselling and Family in IBD: 30 years' Experience at the Cleveland Clinic |
title_sort |
genetic counselling and family in ibd: 30 years' experience at the cleveland clinic |
publisher |
Hindawi Limited |
series |
Canadian Journal of Gastroenterology |
issn |
0835-7900 |
publishDate |
1990-01-01 |
description |
The Cleveland Clinic has followed 1288 patients with inflammatory
bowel disease (IBD) (437 with mucosa! ulcerative colitis and 851 with
Crohn's disease) from 1955 through 1984. Of the 437 patients with mucosal
ulcerative colitis, the index patient had one or more family members develop
IBD. These data indicate the need for the treating physician to institute case-finding
questions within the family so that early diagnoses can be established.
From 1975 through 1984, 94 patients had a positive family history and 63 had
additional family members with disease. The highest risk group was the sibling-sibling
group (6.4% in mucosa! ulcerative colitis and 8.3% in Crohn's disease).
Both groups had similar percentages for all immediate family members; namely,
16.5% and 17.3%. In the group of patients reported from 1975 to 1984, the
location of disease in the index patient and the immediate family member was
the same in 67.5% and different in 30.0%. In this same group of patients, the
disease similarity in the index patient and the immediate family member was the
same in 86.8% and different in 12.0%. These data suggest that while genetic
factors undoubtedly increase the susceptibility for IBD, there is no specific
genetic pattern identified. Also, environmental and other factors may be present.
The data also suggest that the age of onset is a factor, perhaps showing increased
association with a positive family history. |
url |
http://dx.doi.org/10.1155/1990/458980 |
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