Gaucher Disease Clinical Trial
Official title:
A Phase I/II Randomized, Controlled Study of OGT 918 in Patients With Neuronopathic Gaucher Disease
Gaucher disease is an inherited functional deficiency of glucocerebrosidase. This enzyme
breaks down a fatty substance (lipid) called glucocerebroside, which is present in all cells
of the body. When cells renew themselves, the lipids must be broken down and discarded.
Because the enzyme does not function well, the lipid builds up in certain tissues, such as
the liver and spleen. The nervous system is involved as well; memory is impaired and it is
difficult to move the eyes from side to side. It has been shown that repeated infusions of
glucocerebrosidase help break down the stored lipid. However, this treatment does not improve
any neurological symptoms.
A medicine called OGT 918 has been shown to slow the production of the lipid that builds up
in Gaucher disease. It also has been shown to enter the brain. It is hoped that taking OGT
918 will reduce the storage of glycolipids in cells and improve the neurological symptoms of
the disease. This clinical trial seeks to evaluate OGT 918 as a treatment for neuronopathic
Gaucher disease by assessing changes in eye movement velocity. A secondary goal is to assess
the clinical safety and tolerability of OGT 918 therapy.
Up to 30 patients from the National Institutes of Health and the Institute of Child Health
(London) will be randomly assigned to OGT 918 or no treatment for 12 months. Study
participants must be clinically diagnosed with neuronopathic Gaucher disease, 12 years of age
or older, and able to swallow capsules. They must have been stable on ERT for at least 6
months before the study.
Patients receiving OGT 918 will receive a dose of 200 mg OGT 918 three times daily. Data
analysis will be done after 12 months. The study will be extended up to 12 months to collect
safety and efficacy data. All patients who complete the main study and enter the extension
study will receive OGT 918.
During a 4-week screening period, eye movement velocity will be measured. These assessments
will be repeated at months 12 and 24. Also at screening and months 12 and 24, the following
tests will be done: MRI/CT, to measure spleen and liver volume; pulmonary imaging (by X-ray)
and function tests; nerve conduction velocity studies and neuropsychological assessments;
evoked response studies (to measure how the brain conducts electrical messages); and tremor
measurements. Additional assessments for tremor will be conducted at months 6 and 18.
Plasma samples will be obtained every 3 months to measure disease markers and safety
profiles. Proteasome samples will be taken at screening and month 6 to identify proteins that
may be associated with Gaucher disease. Blood will be obtained at month 1 from the first 6
consenting patients who have been randomly assigned to take OGT 918. These patients will also
have a cerebrospinal fluid sample taken by lumbar puncture at month 1. These samples will be
measured for how much OGT 918 is present.
All patients receiving OGT 918 will have an initial assessment 1 week after beginning
treatment to evaluate tolerance of the therapy. Clinic visits will be every 3 months. All
patients will be asked to keep a simple diary of adverse events and dietary information. Dose
levels may be reduced if a patient experiences severe gastrointestinal problems.
Gaucher disease is an inherited functional deficiency of glucocerebrosidase
(beta-glucosidase) which leads to glycolipid accumulation in various tissues. OGT 918 is a
reversible inhibitor of glucosylceramide synthase, a key enzyme in the synthesis of
glycolipids, and has shown beneficial effects in a clinical study in type 1 Gaucher disease.
The primary objective of this clinical trial is to evaluate OGT 918 as a treatment for
neuronopathic Gaucher disease by assessing changes in saccadic eye movement velocity. Other
markers of the disease will also be assessed, including neurological and pulmonary
involvement. Secondary objectives are to assess the clinical safety and tolerability of OGT
918 therapy.
Up to 30 patients, recruited from the National Institutes Health, Bethesda, USA and the
Institute of Child Health, London, U.K. will be randomized to OGT 918 or no treatment in a
2:1 ratio for the 12 month study period. Patients will be clinically diagnosed with
neuronopathic Gaucher disease, 12 years of age or older, on a stable dose of enzyme
replacement therapy (ERT) for at least 6 months and be able to swallow capsules.
Randomization will be stratified based on whether or not the patient has undergone a
splenectomy.
All patients will follow an identical visit schedule. Patients aged 12 years or over
randomized to receive OGT 918 will commence treatment at a dose of 200 mg (2 x 100 mg
capsules) OGT 918 three times daily. As some patients may experience initial gastrointestinal
intolerance this dose may be modified, however the aim will be to maintain patients at the
highest tolerable dose in order to achieve the most clinical benefit. Data analysis is
planned, comparing OGT 918 to the no treatment group, when all patients have completed 12
months of the study. The study will be extended, up to a total of 12 additional months, to
collect safety and efficacy data. The length of the extension study will be dependent on the
results of the final analysis. All patients completing the main study, including those
initially randomized to the no treatment group, will be able to participate in the extension
study unless there are safety issues to prohibit this. All patients in the extension study
will receive OGT 918.
Disease activity assessments will be conducted as indicated in the study flow charts. For a
complete description of all study assessments, please refer to Section 7 of the main
protocol. Where possible, study assessments will be blinded.
The effect of OGT 918 on the electro-oculographic characteristics of saccadic activity,
specifically the amplitude/velocity characteristics (main sequence), will be the primary
outcome variable. Saccadic velocity-amplitude relationship is decreased in neuronopathic
Gaucher patients. This study will assess whether OGT 918 therapy is capable of improving or
stopping any further deterioration of this ocular function.
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