MedPath

Genetic, Serological Fecal and Clinical Markers in Siblings of Children With Inflammatory Bowel Disease

Not Applicable
Completed
Conditions
Inflammatory Bowel Disease
Interventions
Other: sample blood and fecal collection
Registration Number
NCT02181153
Lead Sponsor
University of Roma La Sapienza
Brief Summary

Although the precise etiology of inflammatory bowel disease (IBD) is still unknown, over the last decade active research allowed to gain more precise insights in the pathophysiology of IBD indicating that the chronic inflammation of the intestinal mucosa is directed against the microbiota of the gut in particularly susceptible individuals. Genetic studies and more recently genome-wide association studies (GWAS) have allowed to identify over 70 susceptibility genes which confer an increased risk of developing IBD. In the last years the attention of researchers has shifted to the identification of the early immunological changes that occur already at a preclinical stage of the disease, trying also at identifying the disease before it shows itself. Recently, the ability of a combination of serological markers in predicting the development of IBD has been demonstrated in adults. However, there are no studies evaluating a cohort of children at high risk for the disease, in whom the first immunological changes underlying the development of IBD could be studied, including a combination of genetic, serological, fecal and clinical markers.

The purpose of this study is to evaluate in a population genetically well-characterized, as siblings and twins of patients affected with IBD, early genetic, serologic, fecal and clinical markers of disease, which may be present even years before developing the disease. The identification of these markers in predisposed individuals could help to implement strategies for prevention or early treatment to modify the natural history of IBD.

Detailed Description

This is a multicenter, prospective, study evaluating the role of serological, genetic, fecal and clinical markers in predicting the development of IBD in a high risk population. The study will be divided in two phases. In the first phase the prevalence of genetic, serologic, fecal, clinical risk factors in 100 siblings of children affected with IBD compared to 100 healthy children with no family history for IBD will be evaluated. The estimated duration of the first phase of the study is 12 months. In a second phase, a long-term follow-up (5 years) will be performed in order to evaluate the accidental cases of IBD in this population.

Recruitment & Eligibility

Status
COMPLETED
Sex
All
Target Recruitment
200
Inclusion Criteria
  • siblings of children affected with IBD
  • children without a family history of IBD
Exclusion Criteria
  • age > 18 years
  • age < 6 years
  • concomitant autoimmune disorders

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
patients without family history of IBDsample blood and fecal collectionBlood and fecal samples of 100 healthy children without a family history of IBD will be collected at the day of enrolment. Clinical risk factors for IBD will be also recorded in a case report form
siblings of patients with IBDsample blood and fecal collectionBlood and fecal samples from 100 siblings of children affected with IBD will be collected at the day of enrolment. Clinical risk factors for IBD will be also recorded in a case report form.
Primary Outcome Measures
NameTimeMethod
To evaluate the prevalence of known susceptibility genes for IBD in siblings and twins of patients affected with IBD, compared to controlsone year
To evaluate the prevalence of serological markers of autoimmunity known as risk factors for IBD in siblings and twins of patients affected with IBD, compared to controlsone year
Secondary Outcome Measures
NameTimeMethod
To evaluate the presence and values of fecal markers of colonic inflammation in siblings and twins of patients affected with IBD, compared to controlsone year

Trial Locations

Locations (1)

Department of Pediatrics, Sapienza University of Rome

🇮🇹

Rome, RM, Italy

Related Trials

Research for biomarkers of inflammatory bowel disease. - Investigation of the usefulness of LRG for evaluation of disease condition after adalimumab treatments

Not Applicable
Iwate Medical University Kochi Medical School Hospital Keio University School of Medicine
Updated 10/17/2023

Novel Biomarkers in Inflammatory Bowel Disease

Unknown Status
Assiut University
Posted 2/7/2019
Updated 5/11/2020

Correlation of Genetic Susceptibility Genes to Inflammatory Bowel Disease in Chinese Han Population

Recruiting
Second Affiliated Hospital of Wenzhou Medical University
Posted 10/8/2021
Updated 11/16/2021

Evaluation of Molecular Mechanisms of Non-response to Therapy in Patients With Inflammatory Bowel Disease

RecruitingNot Applicable
Central Hospital, Nancy, France
Posted 2/17/2023
Updated 5/6/2025
© Copyright 2025. All Rights Reserved by MedPath
HomeTerms & ConditionsPrivacy Policy