Overview

Efficacy of Bromopride and Simethicone Versus Bromopride in Functional Dyspepsia

Status:
Completed

Trial end date:
2019-03-11

Target enrollment:
0

Participant gender:
All

Summary

Multi-center, randomized, superiority, double blind clinical trial to asses the efficacy of fixed-dose combination of bromopride and simethicone versus isolated bromopride on research participants diagnosed with functional dyspepsia.

Phase:

Phase 3

Accepts Healthy Volunteers?

Details

Lead Sponsor:

EMS

Treatments:

Bromopride
Metoclopramide
Simethicone

Criteria

Inclusion Criteria:

- Signed Informed Consent;

- Participants aged 18- 70 years;

- Clinical diagnosis of functional dyspepsia according to Rome III criteria;

- Minimum score of 22 points in PADYQ questionnaire

Exclusion Criteria:

- Diagnosis of gastroesophageal reflux disease, irritable bowel syndrome, inflammatory
bowel disease, gallstones, strongyloidiasis, giardiasis or ascariasis, clinical
disease or significant psychological;

- Positive diagnosis for Helicobacter pylori;

- Clinically significant organic diseases in the HDE (High Digestive Endoscopy) prior to
randomization;

- History of esophageal surgery, gastrointestinal or other intra-abdominal surgery;

- Hypersensitivity to the components of the formulations;

- Allergy tartrazine yellow dye;

- Allergy to aspirin;

- Use of PPIs, H2 blockers, prokinetics, antibiotics, prostaglandins or bismuth salts in
the last week before the screening visit;

- Use of NSAIDs or aspirin more than two days a week (except AAS <325mg / day), other
drugs that induce gastrointestinal symptoms;

- Pregnant women or women without adequate contraception;

- Advance Participation in clinical trial protocols in the last twelve (12) months (CNS
Resolution 251 of August 7, 1997, Part III, subsection J), unless the investigator
considers that there may be direct benefit to it;

- Changes in hematological and biochemical tests: hemoglobin less than 12 g / dl,
results with value 2 times the reference for AST, ALT, Gamma GT and alkaline
phosphatase;

- Diagnosis of neurological or psychiatric diseases or decompensated diabetes;

- Use of drugs with anticholinergic action, narcotic analgesics, sedatives, hypnotics or
tranquilizers;

- Alcoholism or sporadic use of alcohol and illicit drug use.