Adenosylcobalamin deficiency
(Redirected from Methylmalonic aciduria, cblA type)
Alternate Names[edit | edit source]
Vitamin B12-responsive methylmalonic acidemia; Vitamin B12-responsive methylmalonic aciduria; Defect in the transport or synthesis of adenosyl-cobalamin
Definition[edit | edit source]
An inborn error of vitamin B12 (cobalamin) metabolism characterized by recurrent ketoacidotic comas or transient vomiting, dehydration, hypotonia and intellectual deficit, which responds to vitamin B12. There are three types: cblA, cblB and cblD-variant 2 (cblDv2).
Epidemiology[edit | edit source]
To date, over 120 patients with cblA, 66 patients with cblB and 6 patients with cblDv2 have been reported. Prevalence of 1/48,000-1/61,000 have been reported for methylmalonic acidemia (MA) of all causes in North America, and 1/26,000 in China, but only a subset of this is vitamin B12-responsive MA.
Cause[edit | edit source]
- Vitamin B12-responsive MA is caused by defects in the synthesis of adenosylcobalamin (AdoCbl).
- There are three distinct complementation classes, cblA, B and Dv2. cblA is caused by mutations in the MMAA gene (4q31.1-2); cblB by the MMAB gene (12q24.1); and cblDv2 by the MMADHC gene (2q23.2).
- The previously reported cblH disorder has been shown to be cblDv2.
Inheritance[edit | edit source]
Transmission is autosomal recessive (1 in 4 recurrence risk/pregnancy).
Signs and symptoms[edit | edit source]
- Patients usually present in infancy or early childhood with features including lethargy, failure to thrive, recurrent vomiting, dehydration, respiratory distress, muscle hypotonia, hepatomegaly and coma. T
- hey may also show signs of anemia (not megaloblastic), have potentially life-threatening ketoacidosis and/or hyperammonemia, and developmental delay and intellectual deficit, with metabolic stroke affecting the brain stem. MA frequently leads to end-stage renal failure by adolescence or adulthood.
- Patients with cblB are usually more severely affected than patients with cblA.
Clinical presentation[edit | edit source]
For most diseases, symptoms will vary from person to person. People with the same disease may not have all the symptoms listed. 80%-99% of people have these symptoms
- Coma
- Dehydration
- Failure to thrive(Faltering weight)
- Hepatomegaly(Enlarged liver)
- Lethargy
- Nausea and vomiting
- Respiratory insufficiency(Respiratory impairment)
30%-79% of people have these symptoms
- Global developmental delay
- Hyperammonemia(High blood ammonia levels)
- Intellectual disability(Mental deficiency)
- Muscular hypotonia(Low or weak muscle tone)
5%-29% of people have these symptoms
- Anemia(Low number of red blood cells or hemoglobin)
- Renal insufficiency(Renal failure)
Diagnosis[edit | edit source]
- Diagnosis is based on increased methylmalonic acid in blood and urine.
- Neonatal screening for propionylcarnitine and/or increased propionylcarnitine-to-acetylcarnitine ratio in dried blood spots by tandem mass spectrometry (MS/MS) has become common, but specific identification of methylmalonic acid remains crucial.
Differential diagnosis Differential diagnoses include MA with homocystinuria , caused by defects in cblC, D and F, which can be differentiated by the presence of megaloblastic anemia, or vitamin B12-unresponsive MA without homocystinuria , which also can present early in life (<1 to 4 weeks) with similar symptoms. Complementation analysis can be used to identify the group involved, or sequencing of the causative genes to identify the affected gene.
Antenatal diagnosis Antenatal diagnosis is possible by measurement of methylmalonate in amniotic fluid and maternal urine at mid-trimester and by studies of functional mutase activity and cobalamin metabolism in cultured amniotic fluid cells. Molecular diagnosis is possible if the gene affected and the mutation(s) in the family are known.
Treatment[edit | edit source]
- Treatment involves a protein-restricted diet, which should be instituted as soon as life-threatening manifestations such as ketoacidosis or hyperammonemia have been resolved, and intramuscular injections of vitamin B12, with or without carnitine (mainly effective in cblA).
- A good response to cobalamin supplementation has been reported in most cblA patients and in nearly half cblB patients.
- Oral antibiotics may also be useful to reduce propionic acid from gut flora.
Prognosis[edit | edit source]
- The prognosis varies with the complement involved, with cblA patients having the most favorable prognosis (most patients well at ages up to 30 years) and cblB patients less favorable.
- cblDv2 appears similar to cblA, although the number of patients is small. One complication in long-term surviving patients is chronic renal failure.
- Treatment involves a protein-restricted diet, which should be instituted as soon as life-threatening manifestations such as ketoacidosis or hyperammonemia have been resolved, and intramuscular injections of vitamin B12, with or without carnitine (mainly effective in cblA).
- A good response to cobalamin supplementation has been reported in most cblA patients and in nearly half cblB patients.
- Oral antibiotics may also be useful to reduce propionic acid from gut flora.
NIH genetic and rare disease info[edit source]
Adenosylcobalamin deficiency is a rare disease.
Adenosylcobalamin deficiency Resources | |
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