Prader-Willi Syndrome Clinical Trial
— TOPRADEROfficial title:
Randomized, Placebo Controlled Double-blind Study of the Efficacy of Topiramate on the Symptoms of Irritability - Impulsivity, Overeating and Self-harm in a Population of Patients Suffering From Prader Willi Syndrome Over 8 Weeks
Verified date | April 2016 |
Source | Assistance Publique - Hôpitaux de Paris |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
There is no specific treatment for core symptoms of PWS. Regarding behavioral and psychiatric
symptoms (hyperphagia, imulsivity and self-mutilations), one of the only drug options
consists in antipsychotics, that are not efficient and might be responsible for a worsening
of the weight gain (major issue in PWS). An alternative therapeutic approach for behavioral
disturbances has been suggested by some authors with topiramate (Epitomax®), an antiepileptic
drug that can be used as a mood stabilizer and anti-impulsive. In addition, topiramate is
used as a treatment for eating disorders because it induces loss of weight and appetite. This
last effect might be useful in the case of SPW.
Except for some clinical case reports, the investigators only found one open study for
topiramate in SPW 8 patientssuggesting promising effects. There si however no placebo
controlled study..
Objective:
To evaluate the efficacy of topiramate (200 mg / d) on Eating disorders (E), self Mutilations
(M), irritability and Impulsivity (I), metabolic status, and tolerance among of PWS patients.
Methodology:
This is a multicenter (out-patients in Toulouse, Reims, Nantes and Paris and in-patients in
Hendaye) 8 weeks double-blind placebo controlled study .
Subjects (n = 125 for 112 analyzable) all having PWS, aged 12 years-old and more should have
any of the following symptoms: E, M and U (see above). All subjects will be randomly
allocated into two groups one taking a placebo, the other taking topiramate (50mg / day
initially, increasing up to 50mg per week 200mg / day).
The population of analyzable patients in and out patient will be of equal size (n = 56). The
inclusion period is two years..
Are excluded subjects with antipsychotic or mood stabilizer medication or topiramate.
The primary endpoint will be the rate of responders, with response defined by obtaining a
score of 1 or 2 on the CGI improvement after 8 weeks of treatment
Other assessments, secondary endpoints :
- Clinic: Weight / Size / Self-injury behavior (french Echelle des Conduites Auto et
Hétéro Aggressives, ECAHA))
- Psychometric: C-SHARP and A-SHARP / Conners (Impulsivity) / Dickens (Eating behavior for
PWS)
- Organic: NFS, serum electrolytes, creatinine, ammonia plasma, serum bicarbonate, AST /
ALT / GGT, ghrelin, fasting glucose, lipid profile and insulin, leptin, TG and HbA1c.
- Side effects of topiramate: SAPS / SANS and BPRS (hallucinations), anxiety scales and
laboratory tests.
Status | Terminated |
Enrollment | 69 |
Est. completion date | June 2016 |
Est. primary completion date | November 2015 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 12 Years to 45 Years |
Eligibility |
Inclusion Criteria: 1. Patient with Prader Willi syndrome confirmed by genetic diagnosis. 2. Patient has at least one of the following symptoms: - Presence of self-harm - Impulsive and / or aggressive - Trouble eating and / or obesity 3. Age between 12 and 45 years inclusive 4. Weight higher than 50 kg 5. Signature of consent by the patient or the holders of parental authority (or legal guardian) Non inclusion criteria: 1. Meeting the criteria according to DSM IV Schizophrenia 2. Presence of hallucination (SAPS scales and scale of hallucination) 3. Already has an effective dose of topiramate for a sufficient time and without efficiency 4. Psychotropic introduced for less than three months or dose change for less than three months. 5. Psychotropic stopped for less than a month, or three months in the case of fluoxetine. 6. Inability to find an informative adult in the subject's behavior. 7. Known hypersensitivity to one of topiramate constituents or its placebo 8. Known hypersensitivity to sulfonamides 9. Epilepsy associated or taking other anticonvulsant or mood stabilizer. 10. Medication with St. John's wort 11. No affiliation to a social security 12. Patient known to be non-compliant 13. Subject to suicide risk 14. Severe depression 15. Previous history of nephrolithiasis or glaucoma 16. Poorly controlled diabetes (A1C greater than 10%) treated with metformin or Gibenclamide. 17. Patients with rare hereditary problems of fructose intolerance, glucose malabsorption or galactose or sucrose-isomaltase insufficiency (because of the presence of sucrose) 18. Pregnant or breastfeeding 19. Lack of effective contraception among patients of childbearing potential Exclusion criteria before randomization: - Renal failure (serum creatinine greater than 1.5 X normal) - Hepatic impairment (ALT greater than 2X normal) ( - Anemia (HB <12 g / dl female <13g / dl man.) - Hyper ammonemia (upper normal laboratory) - Responding to the Schizophrenia criteria according to DSM IV - Presence of hallucination (SAPS scales and scale of hallucination) - Decreased serum bicarbonate levels (below the laboratory standards) |
Country | Name | City | State |
---|---|---|---|
France | Hôpital La Pitié Salpêtrière | Paris |
Lead Sponsor | Collaborator |
---|---|
Assistance Publique - Hôpitaux de Paris |
France,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Clinical Global Impression Improvement | Endpoint CGI score at 1 or 2 will make consider the patient as a responder. A 7 items scale will be used | at 8 weeks (endpoint) | |
Secondary | Weight and size | Weight and size (BMI in kg/m2) | at 8 weeks (endpoint) | |
Secondary | Self-Injury Behavior Scale ECAHA, | Comparison between baseline score and endpoint score | at 8 weeks (endpoint) | |
Secondary | Self-Injury Behavior, CONNERS Impulsivity | CONNERS Impulsivity comparison between baseline score and endpoint score | at 8 weeks (endpoint) | |
Secondary | Self-Injury Behavior,Dickens | Dickens comparison between baseline score and endpoint score | at 8 weeks (endpoint) | |
Secondary | C-SHARP (Chid and Adolescent), appearance of positive suicide item response | at 8 weeks (endpoint) | ||
Secondary | A-SHARP (Adult), appearance of positive suicide item response | A-SHARP (Adult), appearance of positive suicide item response | at 8 weeks (endpoint) | |
Secondary | Safety Assessment | The proportion of patients stopped the treatment, of patients with adverse events and prematurely discontinued treatment due to an adverse event will be estimated. | at 8 weeks (endpoint) | |
Secondary | Biological assessment | The number of patients with abnormal values and / or modified from the baseline values will be evaluated | at 8 weeks (endpoint) |
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