Genetic Disease Clinical Trial
Official title:
Phase 2, Double-Blind, Placebo Controlled Clinical Trial of EPI-743 in Subjects With Cobalamin C Defect
The aim of the research is to investigate the safety and efficacy of EPI-743 treatment in patients with Cbl-C defect and related visual and neurological impairment. Primary Endpoints will be the improvement in visual function as assessed by visual acuity and eye-hand coordination and manual dexterity. Secondary Endpoints will be the improvement in neurologic function, evaluated by a battery of age-appropriated psychophysical tests, and/or in objective electrophysiological tests such as Visual Evoked potentials (VEP) and Electroretinogram (ERG) and/or the change in serum markers of redox state.
Cobalamin C (Cbl-C) defect is the most common inborn error of cobalamin metabolism causing
methylmalonic aciduria and homocystinuria. Cbl-Cdefect is due to impaired activity of
MMACHC, a cobalamin trafficking protein, involved in the decyanation of cyanocobalamin as
well as in the dealkylation of alkylcobalamins through a glutathione transferase activity.
Despite pharmacological treatment with hydroxycobalamin, betaine, folic acid, (and
carnitine), long-term outcome in early-onset patients is in most cases unsatisfactory with
progression of visual and neurological impairment, mainly expressed in the form of retinal
degeneration and/or maculopathy. Moreover, despite some hypotheses have been proposed, the
pathophysiological mechanism causing progressive eye and brain damage still remains unclear.
Recently, the contribution of oxidative stress has been hypothesized based on in vitro
studies showing in Cbl-C fibroblasts a significant increase of reactive oxygen species (ROS)
and in vivo studies documenting severe alteration of glutathione species, the main cellular
redox buffer.
EPI-743 is a small molecule therapeutic that has demonstrated beneficial effects in diseases
characterized by oxidative stress and alterations in glutathione redox balance including
Leigh syndrome and other inherited respiratory chain diseases.
Based on the principle that Cbl-C defect causes both in vivo and in vitro perturbations of
redox state, the aim of our study is to verify the potential beneficial effects of EPI-743
in preventing/reducing progression of neurological and visual signs, as well as in
ameliorating redox abnormalities in Cbl-C patients, in combination with standard therapy.
Primary Endpoints will include the improvement in visual function as assessed by visual
acuity and eye-hand coordination and manual dexterity. Secondary Endpoints will be
improvement in neurologic function, evaluated by a battery of age-appropriated
psychophysical tests, and/or in objective electrophysiological tests such as VEP and ERG,
and/or the change in serum markers of redox state. Patient's and parental Quality of life
will be regularly assessed prior of treatment start and periodically while on EPI-743.
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