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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT04624750
Other study ID # MEX-NM-301
Secondary ID
Status Recruiting
Phase Phase 3
First received
Last updated
Start date September 3, 2021
Est. completion date August 8, 2024

Study information

Verified date May 2024
Source Lupin Ltd.
Contact Nikki Adetoro
Phone 443-447-4534
Email NikkiAdetoro@lupin.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is an open-label, multi-centre, single arm, interventional study to describe the steady-state PK, safety, and efficacy of mexiletine in paediatric patients (6 to <18 years of age) with myotonic disorders.


Description:

This is an open-label, multi-centre, single arm, interventional study to describe the steady-state PK, safety, and efficacy of mexiletine in paediatric patients (6 to <18 years of age) with myotonic disorders. Patients who meet the eligibility criteria will be enrolled stepwise, sequentially in 2 cohorts by age groups. Cohort 1 - Adolescents aged 12 to <18 years, will be enrolled first. If no safety concerns are observed (based on data evaluation by the Data Safety Monitoring Board [DSMB]), and the dose for the age group 6 to <12 years is confirmed by PK model, enrolment for Cohort 2 will begin. Cohort 2 - Children aged 6 to <12 years, will be enrolled. The overall treatment duration for each cohort will be approximately 56 days (8 weeks): a dose titration phase of 4 weeks and the maintenance phase of 4 weeks. The overall study duration would be approximately 22 months. Dose titration phase: In this phase, patients will receive mexiletine starting at an age appropriate dose (as evaluated by the investigator and based on body weight) at a frequency of once a day. Dose will be up-titrated every 14 days based on tolerability of mexiletine up to a maximum of three-times a day as assessed by investigator. Maintenance phase: During the maintenance phase, patients will continue to receive mexiletine at the best-tolerated dose from the titration phase for further 4 weeks. Following completion, all participants will be offered follow-up in PIP Study 7 (MEX-NM-303) (EudraCT: 2019-003758-97).


Recruitment information / eligibility

Status Recruiting
Enrollment 14
Est. completion date August 8, 2024
Est. primary completion date June 24, 2024
Accepts healthy volunteers No
Gender All
Age group 6 Years to 18 Years
Eligibility Inclusion Criteria: 1. Male or female patients aged = 6 and < 18 years who are able to comply with the study requirements 2. A genetically confirmed diagnosis of NDM or DM (DM1or DM2) 3. Presence of clinical symptoms of myotonia (hand grip myotonia, myotonia in the leg muscles, any other myotonia symptoms) 4. No significant cardiac abnormalities as determined by a cardiologist's assessment of the ECG and echocardiogram performed within 3 months prior to enrolment in the study. (If not done within 3 months before trial, electrocardiogram (ECG) and echocardiogram assessments will be performed at screening) 5. No history of any significant liver disorder 6. Patients receiving mexiletine treatment agree to stop treatment at least 7 days prior to initiation of treatment with Namuscla 7. Patients receiving other antimyotonic treatment agree to stop treatment for at least 7 times the half-life of respective drug 8. Laboratory investigations for haematology, biochemistry, and urinalysis at screening are within the normal range, or showing no clinically relevant abnormal values, as judged by the Investigator. 9. Female patients of childbearing potential must be using an acceptable form of birth control as determined by the Investigator (e.g., oral contraception, implantable, injectable/transdermal hormonal contraception, intrauterine device (IUD), barrier methods), tubal ligation or are practicing abstinence. 10. Patients able to provide assent to study participation and a parent or legal guardian to sign the written informed consent prior to study entry. Exclusion Criteria: 1. Any contra-indication to mexiletine as listed in the Namuscla Summary of Product Characteristics (SmPC): 1. Hypersensitivity to the active substance, or to any of the excipients 2. Hypersensitivity to any local anaesthetic 3. Ventricular tachyarrhythmia 4. Complete heart block (i.e., third-degree atrioventricular block) or any heart block susceptible to evolve to complete heart block (first-degree atrioventricular block with markedly prolonged PR interval (= 200 ms) and/or wide QRS complex (= 120 ms), second-degree atrioventricular block, bundle branch block, bifascicular and trifascicular block), 5. QT interval > 450ms 6. Myocardial infarction (acute or past), or abnormal Q-waves 7. Symptomatic coronary artery disease 8. Heart failure with ejection fraction <50% 9. Atrial tachyarrhythmia, fibrillation or flutter 10. Sinus node dysfunction (including sinus rate < 50 bpm) • Co-administration with medicinal products inducing torsades de pointes (class Ia, Ic, III antiarrhythmics): Co-administration of mexiletine and antiarrhythmics inducing torsades de pointesclass Ia: quinidine, procainamide, disopyramide, ajmaline; class Ic: encainide, flecainide, propafenone, moricizine; class III: amiodarone, sotalol, ibutilide, dofetilide, dronedarone, vernakalant) increases the risk of potentially lethal torsades de pointes. 11. Co-administration with medicinal products with narrow therapeutic index 2. Any other neurological or psychiatric condition that might affect the study assessments 3. Any clinically significant illness, laboratory findings, ECG, or other clinical symptoms, which in the opinion of the Investigator could affect the patient's optimal participation in the study 4. Strong inducer or inhibitor of CYP2D6 or CYP1A2 within 7 days prior to study drug administration 5. Any concurrent illness, or medications which could affect the muscle function 6. Seizure disorder, diabetes mellitus requiring treatment by insulin 7. Pregnant or breastfeeding 8. Concurrent participation in any other clinical trial.

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
Mexiletine
Patients will be enrolled sequentially into 2 cohorts. Cohort 1 - (patients aged 12 to < 18 years): approximately 8 weeks - 4 weeks of dose titration period + 4 weeks of maintenance period. Cohort 2 - (patients aged 6 to < 12 years,): approximately 8 weeks - 4 weeks of dose titration period + 4 weeks of maintenance period. Enrolment for Cohort 2 will begin after initial safety assessment of patients in Cohort 1 by the DSMB and no safety concerns are observed. The dose level for cohort 2 will be confirmed by PK modelling study.

Locations

Country Name City State
France Hôpital Necker-Enfants-Malades Paris

Sponsors (1)

Lead Sponsor Collaborator
Lupin Ltd.

Country where clinical trial is conducted

France, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number and frequency of adverse events (AEs)/serious adverse events (SAEs) Number and frequency of adverse events (AEs)/serious adverse events (SAEs), throughout the study while on treatment with Namuscla Baseline to Day 56
Primary Incidence of adverse events of special interest (AESI) Incidence of adverse events of special interest (AESI) Baseline to Day 56
Primary Changes in ECG assessments from baseline On resting ECG any alteration will be noted:
Mild ECG abnormalities: PR interval =200 ms and QRS duration =100 ms
Severe ECG abnormalities: PR interval =240 ms, QRS duration =120 ms, second or third degree AV block and a rhythm other than sinus
Baseline to Day 56
Primary Efficacy of Namuscla treatment on the clinical outcomes based on the following functional evaluation mean change in Visual Analogue Scale (VAS) for muscle stiffness. Mean change in Visual Analogue Scale (VAS) for muscle stiffness. The VAS is constructed as an absolute measure, with a 10 cm straight horizontal line having the endpoints "no stiffness at all" and "stiffness as worst possible". The patient's responses will be scored on the line to the nearest millimetre (a 100-point scale). (myotonia severity). Baseline to Day 56
Primary Efficacy of Namuscla treatment on the clinical outcomes(change from baseline to Days 14, 28, 42 and 56, respectively) based on the following functional evaluation The score of handgrip myotonia as quantitatively measured using a commercially available grip dynamometer and computerised capture system. In standardised conditions (i.e. in a room at controlled temperature, after a definite period of rest), maximum voluntary contractions following forced right hand grip will be recorded and the time to relax from 90% to 5% of maximal force will be determined using automated analysis software Baseline to Day 56
Secondary Mean change in VAS score for muscle pain, weakness and fatigue The VAS is constructed as an absolute measure, with a 10 cm straight horizontal line having the endpoints "no stiffness at all" and "stiffness as worst possible". The patient's responses will be scored on the line to the nearest millimetre (a 100-point scale). The score of stiffness severity as self-reported by the patient on a 10-point VAS will be used for adolescents and children older than 8 years and will be summarised descriptively by visit Baseline - Day 56
Secondary Clinical myotonia assessment for mean change in time to open the eyes Mean change in time to open the eyes after forced eye closure as measured on a stopwatch (when eyelid myotonia present). Subjects will be asked to squeeze their eyes closed for 5 seconds then rapidly open them for 5 seconds then rapidly open. Five trials of each manoeuvre will be performed in sequence at each visit and the time measured on a stopwatch Baseline - Day 56
Secondary Clinical myotonia assessment of clinical change in flexor myotonia Clinical change in flexor myotonia (right hand flexor muscles). Subjects will be asked to make a tight fist for 5 seconds then rapidly open. Five trials of each manoeuvre will be performed in sequence at each visit and the time measured on a stopwatch Baseline - Day 56
Secondary Clinical myotonia assessment of mean change in time to perform Timed-up and go (TUG) test Mean change in time to perform Timed-up and go (TUG) test. Measures, in seconds, the time taken by an individual to stand up from a standard arm chair (approximate seat height of 46 cm, arm height 65 cm), walk a distance of 3 meters (approximately 10 feet), turn, walk back to the chair, and sit down. Baseline - Day 56
Secondary Mean change in health-related quality-of-life as measured by the Paediatric Quality of Life (PedsQL) score Mean change from baseline to Day 56, respectively in health-related quality-of-life as measured by the Paediatric Quality of Life (PedsQL) score. These multidimensional scales assess the frequency of health problems using generic and disease-specific approaches, respectively. Subjects and/or parent or proxies report a score of 0 to 4 (never to almost always) and questionnaires are tailored to age groups. Baseline - Day 56
Secondary Clinical Global Impression (CGI) scores (efficacy and tolerability) evaluated by the patient Clinical Global Impression (CGI) scores (efficacy and tolerability) evaluated by the patient, a parent or proxy and by the investigator at baseline and Day 56. Evaluated on a 4-point scale as very efficient, good, fair or poor. Baseline - Day 56
Secondary Mean change in Myotonia Behaviour Scale (MBS) scores Mean change from baseline to Day 56 in Myotonia Behaviour Scale (MBS) scores The Myotonia Behaviour Scale (MBS) (Hammaren et al., 2005) 0 No stiffness
Some stiffness exists, which can be ignored
Some stiffness exists, which can be ignored at times, but doesn't impair daily activities
Stiffness exists, which demands a higher level of mental awareness when performing some duties and activities
Severe stiffness exists, which impairs every duty and activity
Incapacitating stiffness exists, which demands constant moving not to be totally locked up, with regard to movement
Baseline - Day 56
Secondary Changes in clinical laboratory values for laboratory safety assessments - Potassium Changes in Potassium values from baseline to Day 56. Baseline - Day 56
Secondary Acceptability of the capsule formulation with respect to the swallowability. Acceptability of the capsule formulation with respect to the swallowability. It will be assessed by interviewing patients and their caregivers at Day 56. Baseline - Day 56
Secondary Palatability of alternative administration Palatability of alternative administration (capsule content with milk/juice or sprinkled on food) by 5-point facial hedonic scale correlated with 100-point Visual Analogue Scale (VAS) at each clinic visit Baseline - Day 56
Secondary Changes in clinical laboratory values from baseline to Day 56 for laboratory safety assessments - Changes in Magnesium values Changes in Magnesium values from baseline to Day 56. Baseline - Day 56
Secondary Changes in clinical laboratory values from baseline to Day 56 for laboratory safety assessments - Changes in Sodium values Changes in Sodium values from baseline to Day 56. Baseline - Day 56
Secondary Changes in clinical laboratory values from baseline to Day 56 for laboratory safety assessments - Changes in Calcium values Changes in Calcium values from baseline to Day 56. Baseline - Day 56
Secondary Changes in clinical laboratory values from baseline to Day 56 for laboratory safety assessments - Changes in Chloride values Changes in Chloride values from baseline to Day 56. Baseline - Day 56
Secondary Mean change in Faces scale for muscle pain, weakness and fatigue A Faces (or other symbol) scale for children aged 6 to 8 years will be used to measure the score of muscle stiffness (myotonia severity). Faces scale will be used to assess pain, weakness and tiredness in study participants with a 10 cm straight horizontal line having the endpoints "no [symptom] at all" and "[symptom] as worst possible" Baseline - Day 56
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