Celiac Disease in Children Clinical Trial
Official title:
Effect of Acetaminophen Versus Ibuprofen in Treating Recurrent Apthous Ulcers in Pediatric Celiac Disease: A Randomized Pilot Study
Celiac disease (CD) is a chronic autoimmune enteropathy. It results from genetic predisposition and exposure to gluten-containing food. Individuals carrying human leucocytes antigen (HLA) markers DQ2 or DQ8 are genetically predisposed. Gluten is a protein found in wheat, rye, and barley; the main ingredients of bread, pasta, and pastries. Gluten works as a triggering factor for CD, but the interaction between genetic and environmental factors is still not fully understood. Celiac disease can alter the absorption of drugs. Due to its vast surface area compared with the stomach, most drug absorption occurs in the small intestine and in celiac disease; the surface area available for absorption is substantially reduced due to villous atrophy. Patients with celiac disease develop a variety of gastric disorders requiring oral medications, but the impact of damage to intestinal villi and other celiac disease squeal on drug absorption remains poorly understood. A review of the pertinent literature (English-language articles on research in adults published during the period 1970-August 2012) identified several reports of altered drug absorption mechanisms in patients with celiac disease, including accelerated or delayed gastric emptying, increased permeability of jejunal mucosa, changes in intraluminal pH, decreased intestinal surface area, and reduced intestinal cytochrome P-450 enzymes. A small number of published studies suggest that celiac disease may be associated with altered drug absorption, resulting in higher serum concentrations of propranolol, lower peak concentrations of acetaminophen and practolol, higher dosing requirements with levothyroxine, impaired or delayed absorption of certain antibiotics, and other pharmacokinetic effects with a potential impact on medication efficacy and toxicity. However, these studies involved very small patient samples and were poorly controlled, with some yielding contradictory results. More and larger pharmacokinetic studies in patients with celiac disease-especially studies of drugs that are dosed empirically or are not amenable to dosage adjustment according to vital signs or laboratory values-are needed.
Status | Not yet recruiting |
Enrollment | 12 |
Est. completion date | December 1, 2024 |
Est. primary completion date | September 1, 2024 |
Accepts healthy volunteers | Accepts Healthy Volunteers |
Gender | All |
Age group | 4 Years to 15 Years |
Eligibility | Inclusion Criteria: - 1. Children with clinical diagnosis with a celiac disease. 2. presence of recurrent apthous ulcers. Exclusion Criteria: - 1. History of allergy to any ingredient present in the drugs to be used for treatment. 2. Children whose parents had no home or mobile phone to enable post-operative contact. 3. Parent that who refuse to sign the informed consent. |
Country | Name | City | State |
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n/a |
Lead Sponsor | Collaborator |
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Cairo University |
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | change in pain intensity | faces pain scale score (from no pain [score 0] to maximum pain intensity [score 10] ) | 6 month | |
Secondary | presence of recurrent apthous ulcer | clinical observation complement by history from parents by yes or no | baseline, before intervention | |
Secondary | Occurrence of Dental enamel defects (DED) | Aine ' s classification of dental enamel defect score (0-4) dental enamel defects | baseline, before intervention | |
Secondary | Dental caries experience | CAST index (score"0: sound", "1: sealant", "2: restoration", "3: enamel lesions", "4,5: dentine lesions", "6: pulp involvement", "7: abscess/fistula", "8: tooth loss". if a situation did not match any code from 0 to 8, a code 9 was assigned.)
l |
baseline, before intervention | |
Secondary | Delayed dental eruption | number of teeth with delayed eruption | baseline, before intervention |
Status | Clinical Trial | Phase | |
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