Prucalopride Versus Placebo in Gastroparesis

Last updated: October 6, 2020
Sponsor: University of Calgary
Overall Status: Completed

Phase

2/3

Condition

Diabetes And Hypertension

Gastroparesis

Diabetes Prevention

Treatment

N/A

Clinical Study ID

NCT02031081
PruGP
  • Ages 18-64
  • All Genders

Study Summary

The incidence of gastroparesis has been increasing among Canadians. Symptoms of discomfort include early satiety, stomach pain, nausea and vomiting. In addition, because gastroparesis slows digestion, it can lead to malnutrition and make controlling blood sugar even more challenging for diabetics. Mild cases of gastroparesis can be helped with dietary and lifestyle modifications but treatments for more severe symptoms are limited. There are several drugs called pro-kinetics available in Canada though results vary among patients and these often cause significant side effects. Recently, a drug called Prucalopride was approved for use in Canada to treat constipation. It has pro-kinetic properties and has been shown to cause few side effects. The investigators propose to test prucalopride as a treatment for gastroparesis by recruiting 30 patients from the Calgary area who have gastroparesis. The investigators will test the effects of this treatment by alternating 28 days of active treatment with prucalopride with 28 days of treatment with a non active placebo adding a two week break in between treatments. The order of the treatment will be randomized and neither the patients nor the investigators will know whether they are receiving the active treatment or the placebo until the study has been completely finished. The investigators will measure the effects using questionnaires that assess patient symptoms such as nausea and pain as well as quality of life during two gastric emptying tests and throughout the treatment periods. The effectiveness of the active treatment will be evaluated by comparing the extent of the change in symptoms before and after treatments and the difference in gastric emptying times as compared to the placebo treatment. The investigators will also monitor and track all possible side effects that patients experience during the study.

Study Hypotheses

In patients with gastroparesis:

  1. Prucalopride 4 mg daily improves meal-related symptoms compared to placebo as defined by the change in cumulative meal-related symptoms. (primary endpoint).

  2. Prucalopride 4 mg daily accelerates gastric emptying rate compared to placebo. (secondary endpoint).

  3. A correlation exists between the effect of prucalopride on gastric emptying rate and symptom improvement.

Eligibility Criteria

Inclusion

Inclusion Criteria:

  • Age of 18-64 years

  • Existing clinical diagnosis of gastroparesis for at least one year as judged by thestudy gastroenterologist based on past medical history, clinical symptoms

  • Sufficiently symptomatic at time of proposed study (Minimum baseline postprandialsatiety/fullness subscale of the Gastroparesis Cardinal Symptoms Index (GCSI) score of 1.5 or higher)

  • Delayed gastric emptying (>10% retention at 4 hours) on standard solid mealscintigraphic emptying study within the previous year

  • Normal upper endoscopy (with the exception of small bezoars) since the onset ofsymptoms

  • If female of childbearing potential, a negative urine pregnancy test administeredbetween consent and screening appointments

  • Able to provide written informed consent

Exclusion

Exclusion Criteria:

  • Clinical evidence (including physical exam and/or ECG) of significant cardiovascular,respiratory, renal, hepatic, gastrointestinal, hematological, neurological,psychiatric or other disease that may interfere with the objectives of the studyand/or pose safety concerns, including pregnancy or breastfeeding.

  • Study entry ECG showing second or third degree heart block, left bundle branch block (LBBB) or acute ischemic changes

  • Blood electrolytes (Na, K, CL) measured within past 6 months outside of normalreference ranges (except during an acute gastroparesis flare-up)

  • Use of narcotics or promotility agents which cannot be stopped prior to study entry.

  • Use of tricyclic antidepressants (at doses exceeding 25 mg/day) and/or macrolideantibiotics. (Stable doses of SSRI/SNRI antidepressants and/or non-macrolideantibiotics are permitted)

  • Laxative use that cannot be stopped prior to the start of the study

  • Participated in clinical trial with motility agents within past 30 days

  • History of gastrointestinal surgery excepting appendectomy and/or cholecystectomy inthe past, or any other major surgeries within 3 months

  • Estimated GFR<30 measured within past 6 months.

  • History of cardiovascular disorder including myocardial infarction, pacemaker orimplanted defibrillator, or history of life-threatening arrhythmia

Study Design

Total Participants: 15
Study Start date:
March 01, 2014
Estimated Completion Date:
June 30, 2018

Connect with a study center

  • University of Calgary

    Calgary, Alberta T2N 4Z6
    Canada

    Site Not Available

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