Evolution of Pediatric Inflammatory Bowel Disease Unclassified (IBD-U): Incorporated With Serologica...
Evolution of Pediatric Inflammatory Bowel Disease Unclassified (IBD-U): Incorporated With Serological and Gene Expression Profiles
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Author / Creator
Chandradevan, Raguraj , Hofmekler, Tatyana , Mondal, Kajari , Harun, Nusrat , Venkateswaran, Suresh , Somineni, Hari K , Ballengee, Cortney R , Kim, Mi-Ok , Griffiths, Anne , Noe, Joshua D , Crandall, Wallace V , Snapper, Scott , Rabizadeh, Shervin , Rosh, Joel R , Walters, Thomas D , Bertha, Madeline , Dubinsky, Marla C , Denson, Lee A , Sauer, Cary G , Markowitz, James F , LeLeiko, Neal S , Hyams, Jeffrey S and Kugathasan, Subra
Publisher
US: Oxford University Press
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Language
English
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Publisher
US: Oxford University Press
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Contents
Abstract
Background
Inflammatory bowel disease (IBD) mainly consists of Crohn's disease (CD) and ulcerative colitis (UC). About 10%-15% of patients with IBD cannot be firmly diagnosed with CD or UC; hence, they are initially diagnosed as inflammatory bowel disease unclassified (IBD-U). Having a firm diagnosis is clearly preferred to guide treatment choices, and better understanding of the nature of IBD-U is required.
Methods
We performed an analysis of a subset of pediatric subjects from an inception IBD cohort of patients initially enrolled in a prospective multicenter study (the RISK study). Initial diagnosis and 2-year follow-up data from the subjects diagnosed with IBD-U were analyzed. An expert panel verified final diagnosis using predefined criteria as a guide. Serological and disease-relevant ileal and rectal tissue gene expression profiles were investigated. The use and the time to initiate anti-TNFα treatment was analyzed among the outcome groups.
Results
A total of 1411 subjects were enrolled with initial diagnosis of IBD, and among them, 136 subjects were initially diagnosed as IBD-U at enrollment. And 26% were reclassified as UC and 14% as CD within 2 years of diagnosis, while 60% remained as IBD-U. Of those who were reclassified, there was a 2:1 ratio, UC (n = 35) to CD (n = 19). The molecular and serological features of IBD-U at the end of follow-up were very similar to UC and very different from CD. There was less likelihood of receiving anti-TNFα agents if the diagnosis was IBD-U compared with CD (P < 0.0001).
Conclusions
In our cohort, 60% of the IBD-U subjects remained as unclassified at 2 years; of those subsequently classified, a higher percentage followed a course more similar to UC. Most of the IBD-U subjects at diagnosis had serological and molecular signatures that are very similar to UC. Although the atypical presentations made the clinician to make an interim diagnosis of IBD-U, results of the molecular and serological factors performed at the time of diagnosis suggests that they were very similar to UC. However, long-term studies are needed to better understand the natural history and molecular characterization of pediatric onset IBD-U.
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Alternative Titles
Full title
Evolution of Pediatric Inflammatory Bowel Disease Unclassified (IBD-U): Incorporated With Serological and Gene Expression Profiles
Authors, Artists and Contributors
Author / Creator
Hofmekler, Tatyana
Mondal, Kajari
Harun, Nusrat
Venkateswaran, Suresh
Somineni, Hari K
Ballengee, Cortney R
Kim, Mi-Ok
Griffiths, Anne
Noe, Joshua D
Crandall, Wallace V
Snapper, Scott
Rabizadeh, Shervin
Rosh, Joel R
Walters, Thomas D
Bertha, Madeline
Dubinsky, Marla C
Denson, Lee A
Sauer, Cary G
Markowitz, James F
LeLeiko, Neal S
Hyams, Jeffrey S
Kugathasan, Subra
Identifiers
Primary Identifiers
Record Identifier
TN_cdi_proquest_miscellaneous_2049941186
Permalink
https://devfeature-collection.sl.nsw.gov.au/record/TN_cdi_proquest_miscellaneous_2049941186
Other Identifiers
ISSN
1078-0998
E-ISSN
1536-4844
DOI
10.1093/ibd/izy136
