Methylmalonic Acidemia (MMA) Clinical Trial
Official title:
Long-term Outcome of N-Carbamylglutamate Treatment in Propionic Acidemia and Methylmalonic Acidemia
Background: Very few drugs exist that treat hyperammonemia, specifically PA and MMA. Diet
restrictions and alternate pathway agents are the current primary treatments, but they
frequently fail to prohibit brain damage.
Orthotopic liver transplantation cures the hyperammonemia of urea cycle disorders, but organ
availability is limited and the procedure is highly invasive and requires life-long
immunosuppression.
A drug that could repair or stimulate a dysfunctional urea cycle such as this would have
several advantages over current therapy. A drug called N-carbamyl-L-glutamate, Carglumic
acid (NCG or Carbaglu)has recently been found to be virtually curative of another urea cycle
defect called NAGS deficiency. In this disorder, treatment with NCG alone normalizes
ureagenesis, blood ammonia and glutamine levels, allows normal protein tolerance and
restores health. Knowledge from this study is being applied to acquired hyperammonemia,
specifically in patients with propionic PA and MMA, to try and improve neurodevelopmental
outcomes by improving the hyperammonemia.
Aims: The overall objective of this project is to determine whether treatment of acute
hyperammonemia with Carglumic acid in propionic acidemia (PA), methylmalonic acidemia (MMA)
changes the long-term outcome of disease and to determine if it is effective in restoring
urine ammonia levels to normal levels.
Methods/Design This 5-year, Phase II, double-blind study aims to recruit and enroll 34 PA
and MMA patients during acute episodes of hyperammonemia.
The primary aim is to circumvent the long-term neurodevelopmental decline due to having a
prolonged levels of ammonia during crisis in the blood and urine. After treatment and crisis
resolution with Carbaglu or placebo and standard of care therapy, measures of
neurodevelopmental outcomes (Bayley II and Functional Status Scale) are being measured at 9,
15,21 and 30 months post-discharge from the hospital. Safety of NCG treatment will also be
monitored as measured by close examination of adverse events and laboratory blood tests. To
test for the effectiveness of NCG, longitudinal models to evaluate the groupwise difference
(NCG vs. Placebo) in the trajectory of change in neurodevelopmental outcomes and safety
analyses between drug and placebo patients.
Subsequent Episodes At any time after the initial episode, participants may present to the
hospital with PA- or MMA-associated symptoms. If the plasma ammonia level verified as a
bonafide episode of HA (plasma ammonia is ≥ 100 µmol/l), that participant will receive the
same study medication that they received during their initial episode in a double-blinded
fashion, (i.e. If the participant received NCG at the time of initial randomization, he/she
will continue to receive NCG at each subsequent HA episode. If the participant received PLBO
at the time of initial randomization, he/she will continue to receive PLBO at each
subsequent HA episode). Only the pharmacist will know if the participant receives NCG or
PLBO. The same study assessments (previously stated) will be conducted at each qualifying
HSA episode.
;
Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Withdrawn |
NCT03810690 -
Open Label Study of mRNA-3704 in Patients With Isolated Methylmalonic Acidemia
|
Phase 1/Phase 2 | |
| Suspended |
NCT05778877 -
A Study to Evaluate the Safety, Tolerability, and Pharmacodynamics of SEL-302 in Pediatric Subjects With MMA
|
Phase 1/Phase 2 |