A Phase 3 Study of UX003 Recombinant Human Betaglucuronidase (rhGUS) Enzyme Replacement Therapy...
MPS 7Sly Syndrome2 moreThe Phase 3 study will use a novel randomized, intra-subject placebo-controlled, single crossover design, referred to as Blind Start, to evaluate the safety and efficacy of UX003. The Blind Start is a novel design whereby participants will be randomized to 1 of 4 groups, each representing a different treatment sequence, and will cross over to UX003 at different pre-defined time points in a blinded manner. All groups will receive a minimum of 24 weeks treatment with 4 mg/kg UX003 every other week (QOW).
Longitudinal Studies of Brain Structure and Function in MPS Disorders
Mucopolysaccharidosis Type IMucopolysaccharidosis Type II3 moreNeurobehavioral function and quality of life are compromised in many patients with mucopolysaccharidosis (MPS) disorders. The long-term goals of this research are to: 1) more accurately inform patients/parents regarding potential neurobehavioral outcomes; 2) develop sensitive measures of disease progression and central nervous system (CNS) treatment outcome; and 3) help clinical researchers develop direct treatments for specific brain structures/functions. The investigators hypothesize that specific and localized neuroimaging and neuropsychological findings and their relationship will be distinct for each MPS disorder. It is further hypothesized that without treatment, functions will decline and structure will change over time in a predictable fashion, and will be related to locus of abnormality and stage of disease.
Biomarker for Sly Disease (MPS VII) (BioSly)
Developmental DelaySkeletal Abnormalities2 moreDevelopment of a new MS-based biomarker for the early and sensitive diagnosis of Sly disease from blood (plasma)
Expanded Access to Mepsevii
MPS VIIMucopolysaccharidosis VII1 moreIndividual patient expanded access requests may be considered for patients who have no other treatment options