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Established genetic risk factors do not distinguish early and later onset Crohn's disease

โœ Scribed by Jonah B. Essers; Jessica J. Lee; Subra Kugathasan; Christine R. Stevens; Richard J. Grand; Mark J. Daly


Book ID
102268108
Publisher
John Wiley and Sons
Year
2009
Tongue
English
Weight
151 KB
Volume
15
Category
Article
ISSN
1078-0998

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โœฆ Synopsis


Background:

Early-onset disease is frequently examined in genetic studies because it is presumed to contain a more severe subset of patients under a higher influence of genetic effects. In light of the dramatic success of Crohn's disease (CD) gene discovery efforts, we aimed to characterize the contribution of established common risk variants to pediatric CD.

Methods:

Using 35 confirmed CD risk alleles, we genotyped 384 parent-child trios (mean age of onset 11.7 years) along with 321 healthy controls. We performed association tests on the independent pediatric cohort and compared results to those previously published. 1 We also computed a weighted CD genetic risk score for each affected person. Six variants not previously validated in children (at 5q33, 1q24, 7p12, 12q12, 8q24, and 1q32) were significantly associated with pediatric CD (P ฯฝ 0.03).

Results:

We detected no significant association between risk score and age at onset through age 30. This analysis illustrates that the genetic effect of established CD risk variants is similar in early and later onset CD.

Conclusions:

These results motivate joint analyses of genomewide association data in early and late onset cohorts and suggest that, rather than established risk variants, independent variants or environmental exposures should be sought as modulators of age of onset.


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## Background: The incidence of Crohn's disease (CD) with onset before age 16 has increased. Several perinatal characteristics have been associated with CD. Our objective was to examine the temporal change in CD incidence by period of birth and the extent that this could be attributed to perinatal