Sodium Valproate for GSDV

University College London (UCL)

Status and phase

Completed

Phase 2

Conditions

Glycogen Storage Disease Type V

McArdle Disease

Treatments

Drug: Sodium Valproate

Study type

Interventional

Funder types

Other

Identifiers

NCT03112889

11/0090

Details and patient eligibility

About

McArdle disease is a metabolic myopathy characterised by the absence of glycogen phosphorylase in skeletal muscle. Sodium Valproate is part of a group of drugs known as histone deacetylase inhibitors, which have a direct effect on chromatin. Recently a drug trial in an animal model of McArdle disease showed that sodium valproate stimulated the expression of a different isoform of the missing enzyme in skeletal muscle.

A safety and feasibility study of sodium valproate in people with McArdle disease has been carried out in London (UK) and Copenhagen (DK) since January 2015. Participants will receive 20mg/Kg/day of sodium valproate for 6 months. The primary outcome measure is exercise performance assessed by cycle ergometry. Pre and post-treatment skeletal muscle biopsies will be performed to assess for glycogen phosphorylase. Together with blood analyses for safety. Additional functional exercise tests will be performed.

Full description

McArdle disease (Glycogen storage disease type V, GSDV) is an inherited metabolic disorder of skeletal muscle. Affected patients are unable to perform strenuous exercise due to a congenital absence of the enzyme muscle glycogen phosphorylase, essential for glycogen metabolism. This enzyme deficiency results in the inability to mobilise muscle glycogen stores from muscle, required for energy during strenuous exercise. In affected people symptoms of fatigue and cramps occur within minutes of initiating any activity and during strenuous activity such as lifting heavy weights or walking uphill, if activity is continued despite severe cramping, a contracture occurs which leads to muscle damage (rhabdomyolysis), myoglobinuria (dark brown/black discolouration of urine) and, when severe, acute renal failure.

Currently no satisfactory treatment can be recommended other than aerobic exercise. Although most people with McArdle disease have complete absence of skeletal muscle phosphorylase, there are a small minority of patients who possess splice site mutations that enable production of very small amounts (1-2%) of functional enzyme. These people have a milder phenotype with less severe symptoms, and functional exercise assessments have shown better exercise capacity than typical patients with the condition. Findings from these atypical individuals suggest potential therapeutic agents might only need to produce very small amounts of enzyme for significant functional improvement. Furthermore, finding a therapeutic agent to 'switch on' expression of the foetal isoenzyme may be a potential therapeutic strategy. There is some evidence from animal studies to suggest that sodium valproate can 'switch on' the foetal phosphorylase isoenzyme. The current proposes to undertake a feasibility study of 8 participants recruited in the UK and 7 in Denmark.

Enrollment

8 estimated patients

Sex

All

Ages

18 to 64 years old

Volunteers

No Healthy Volunteers

Inclusion criteria

Male subjects and post-menopausal or infertile females
Diagnosed with GSDV and over 18 years of age
Normal serum carnitine level and acylcarnitine blood profile at screening visit

Exclusion criteria

Children under the age of 18 years
People older than 64 years
Females of child bearing potential
Patients with Diabetes
Inflammatory disorders especially systemic lupus erythematosis.
A previous history of sensitivity/allergy to sodium valproate and its excipients
Patients treated with sodium valproate for epilepsy or a psychiatric disorder within the last 12 months prior to screening
Patients with pre-existing liver disease or a family history of severe liver disease affecting a first degree relative. Liver disease will be defined by abnormal liver biopsy. Patients with GSDV may have raised serum transaminases that originate from muscle but which may cause abnormal liver function tests measured in serum, this will not be a reason for exclusion.
Patients prescribed other anti-convulsant medication or any other medication known to interact with sodium valproate (see section 9.3).
Patients who are sensitive to local anaesthetics that would prevent muscle biopsy.
Subjects with any co-morbid illness or disability which would prevent an exercise assessment such as severe unstable/ untreated ischaemic heart disease, lower limb disability such as severe muscle weakness with muscle strength assessed as worse than MRC scale 3 in any pelvic girdle muscle.
Inability to exercise due to a lower limb fracture would be an exclusion criterion until there is complete recovery of the injury.
Patients known to have porphyria or an affected first degree relative affected with porphyria will be excluded from the study.
Patients known to have mitochondrial disease or where there is a first degree relative with mitochondrial disease.
Patients with a history of abnormal acyl carnitine profile or low serum carnitine level
Male participants unwilling to use contraception