Clinical Importance of Carrier Status of Recessive Gene Mutations in Myopathy (CICS) (CICS)
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|ClinicalTrials.gov Identifier: NCT02897921|
Recruitment Status : Not yet recruiting
First Posted : September 13, 2016
Last Update Posted : September 14, 2016
Many myopathies are inherited in a recessive manner, but in some of these recessively inherited disorders, clinical manifestations may potentially manifest in carriers of just a single mutation.
The aim of the study is to describe the clinical characteristics of single mutation carriers of recessive myopathy, through measuring serum creatine kinase, muscle strength, muscle degeneration (by MRI) and heart affection. The investigators will do this by blood sampling, Biodex 4 Isokinetic Dynamometer, MRI analysis, ECG, Holter monitoring, and echocardiography.
The aim is further to describe whether these characteristics are found primarily with specific mutations.
|Condition or disease|
|Recessive Gene Myopathies|
Many myopathies are inherited in a recessive manner, but in some of these recessively inherited disorders, clinical manifestations may potentially manifest in carriers of just a single mutation. This has recently been demonstrated by researchers for the recessively inherited limb girdle muscle dystrophy (LGMD) type 2A, where carriers of single mutations can also be symptomatic. In X-linked recessively inherited dystrophinopathies caused by mutations in the DMD gene on chromosome Xp21, female mutation carriers may also manifest with disease, although this is often milder than affected men. In the recently discovered LGMD2L, manifesting carriers are also suspected. Thus, according to statistics, too many persons evaluated for myopathy carry a single LGMD2L mutation.
Some previous studies have looked into the significance of being a single mutation carrier in recessive muscle disease. In dystrophinopathy, it was reported that 5 % of female DMD carriers reported myalgia and cramps, 17 % experienced mild-to-moderate muscle weakness and 8 % experienced dilated cardiomyopathy, with a mean onset age of approximately 30 years. Another study found that echocardiographic examination was abnormal in up to 38% of DMD female carriers - some with dilated cardiomyopathy, and some with left ventricle dilatation.
Overall, however significance of carrying a single mutation of recessive myopathy is widely unexplored. No study has yet investigated the characteristics of single mutation carriers of recessive myopathy in an observational, cross-sectional study.
In this study, clinical characteristics of single mutation carriers of recessive myopathies will be investigated. The investigation will include sceletal muscle degeneration and strength, as well as cardiac status.
Recruitment and Methods:
Estimated total of subjects recruited is 200 with known recessive gene mutations, and 40 healthy controls. In former studies 40 healthy volunteers have already been investigated, thereby giving a total of 80 healthy controls. Recessive gene carrier recruits will be obtained via the Department of Clinical Genetics and Copenhagen Neuromuscular Center, Rigshospitalet, thus only including carriers aware of their carrier status.
2 days of testing per participant. Day one: Measuring S-creatine kinase level (blood sampling), muscle strength (Biodex 4 Isokinetic Dynamometer), ECG, and Holter monitor device application.
Day two: Holter monitor device removal, Dixon MRI analysis with gadolinium contrast medium, and echocardiography.
Healthy controls will take part in MRI-scanning and isokinetic dynamometer testing.
Trials are expected to be carried out between October 2016 and May 2020.
|Study Type :||Observational|
|Estimated Enrollment :||240 participants|
|Observational Model:||Case Control|
|Official Title:||Clinical Importance of Carrier Status of Recessive Gene Mutations in Myopathy|
|Study Start Date :||October 2016|
|Estimated Primary Completion Date :||May 2020|
|Estimated Study Completion Date :||August 2021|
Carriers of recessive gene mutations of myopathies
Patients with several different kinds of recessively inherited myopathy genes, such as for example Duchenne's Muscular Dystrophy, Becker's Muscular Dystrophy, Limb Girdle limb girdle muscle dystrophy (LGMD) type 2A and 2L etc.
Investigated by blood sampling, Biodex 4 Isokinetic Dynamometer, MRI analysis, ECG, Holter monitoring, and echocardiography.
Healthy controls, investigated by blood sampling, Biodex 4 Isokinetic Dynamometer and MRI analysis.
- Cardiac status [ Time Frame: MRI of cardiac status and muscles takes around 1,5 hours ]We will use MRI with a contrast agent (gadolinium). Kidney function and contrast allergy status will be tested prior to use of contrast agent, and avoided if the participant is not suitable for contrast injection.
- Muscle tissue quality [ Time Frame: MRI of cardiac status and muscles takes around 1,5 hours ]Muscle tissue cross sectional area and fat percent will be investigated and measured by Dixon MRI scan.
- Serum CK-levels [ Time Frame: Estimated time 5 minutes. ]Blood sampling
- Muscle strength [ Time Frame: Testing takes around 10-20 minutes ]Investigated by an isokinetic dynamometer (Biodex 4).
- ECG [ Time Frame: Estimated time: 5 minutes. ]ECG electrodes will be places on the subject's chest, and an electrocardigram will be measured.
- Holter monitor [ Time Frame: A Holter monitor device will be attached on test day 1, and worn until test day 2 (24-48 hours) ]The electrodes will be places on the chest and the monitor attached in a line around the neck. 24-48 hours of electrocardiogram will be measured.
Biospecimen Retention: Samples With DNA
To learn more about this study, you or your doctor may contact the study research staff using the contact information provided by the sponsor.
Please refer to this study by its ClinicalTrials.gov identifier (NCT number): NCT02897921
|Contact: Tove Freja M Fornander, B. Sc.||35456135 ext firstname.lastname@example.org|
|Contact: Nanna S Nielsen, B. Sc.||35456135 ext 45||Nanna.email@example.com|
|Copenhagen Neuromuscular Center, Rigshospitalet, 3342|
|Copenhagen, Denmark, DK-2100|
|Principal Investigator:||Tove Freja M Fornander, B. Sc.||Copenhagen Neuromuscular Center|