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DRUG REACTIONS clinical trials

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NCT ID: NCT03659227 Recruiting - Clinical trials for Stevens-Johnson Syndrome

Drug Reactions Sampling (COLLECTIONTOXIDERMIES)

Start date: September 26, 2018
Phase:
Study type: Observational

Intro: Dermatology department of Henri Mondor Hospital (Creteil, France), is a reference center for toxic bullous diseases and severe cutaneous drug reactions (Stevens-Johnson syndrome (SJS), Lyell syndrome (toxic epidermal necrolysis (TEN)), generalized bullous fixed drug reactions, AGEP, DRESS, drug induced immunoglobulin A (IgA) bullous dermatosis, and erythema multiforme). In order to conduct clinical and biological research studies in drug reactions, it is necessary for the investigator's department to implement a collection of clinical data and biological samples. Hypothesis/Objective: To collect clinical data and cutaneous and biological samples for immunological, biological and genetic studies to improve knowledge about pathophysiology of drug reactions. Method: The following samples will be performed in addition to the routine practice samples: one skin punch biopsy (6mm); 43 mL of blood; blister fluid aspiration; oral and nose mucous membrane and skin eSWABs, stool samples. These samples will be stored in a dedicated biological sampling department ("Platform of biological resources"). Conclusion: The implementation of this collection should allow us to conduct pathophysiological studies about drug reactions.

NCT ID: NCT03195946 Completed - Drug Reactions Clinical Trials

Effects of Repeated Doses of Lu AF35700 on Drug Metabolizing Enzymes

Start date: June 16, 2017
Phase: Phase 1
Study type: Interventional

This study will help determine which types of drugs that may interact with Lu AF35700

NCT ID: NCT01775839 Completed - DRUG REACTIONS Clinical Trials

Clinical Trial to Evaluate the Influence of Genotype and DDIs of Aspirin on the PK/PD of Clopidogrel and PK of Digoxin

Start date: January 2013
Phase: Phase 4
Study type: Interventional

Clinical trial to evaluate the influence of multiple aspirin administration on PK and PD of co-administered drugs