Abstract

BackgroundThe cblC defect is a rare inborn error of intracellular cobalamin metabolism. Biochemical hallmarks are elevated homocysteine and low methionine in plasma accompanied by methylmalonic aciduria. Due to the heterogeneous clinical picture, patients with the late-onset form of the disease (onset >12 months) come to the attention of diverse medical specialists, e.g. paediatricians, neurologists, nephrologists, psychiatrists or haematologists. The report reviews the published clinical data and adds three new cases to raise awareness for this severe but often treatable disease.MethodsThe Pubmed and the Cochrane databases were searched for clinical reports on cblC patients and three unreported cases are presented to illustrate the clinical spectrum.ResultsReports on 58 cases (30 females, 22 males, 6 = no information) and the three new cases underlined the clinical heterogeneity of the disease. Time between first symptoms and diagnosis ranged from three months to more than 20 years. Haemolytic uraemic syndrome and pulmonary hypertension were main presenting symptoms in preschool children. In older children/adolescents, psychiatric symptoms, cognitive impairment, ataxia and myelopathy were frequently observed while thromboembolic events and glomerulopathies were almost exclusively seen in adults. Brain atrophy, white matter lesions and myelopathy were frequently encountered. The majority of patients showed marked biochemical and clinical response to treatment with parenteral hydroxocobalamin combined with oral betaine, folate, carnitine and rarely methionine. The course was less favourable in late treated or untreated patients.ConclusionsThe late-onset cblC defect is a rare disease and unfortunately, diagnosis is often delayed. Raising awareness for this disorder can significantly improve patients’ outcome and perspective by timely initiation of targeted treatment. Newborn screening (NBS) for the cblC defect might be of benefit especially for late-onset patients since treatment seems efficient when initiated before irreversible organ damage. In general, inborn errors of metabolisms should be considered in unexplained medical cases at any age, especially in patients with multisystemic disease. More specifically, total homocysteine in plasma and methylmalonic acid in urine/plasma should be measured in unexplained neurologic, psychiatric, renal, haematologic and thromboembolic disease.

Highlights

  • The Cobalamin C (cblC) defect is a rare inborn error of intracellular cobalamin metabolism

  • The cblC defect (ORPHA 79282; MIM 277400) is an inborn error of intracellular cobalamin metabolism caused by mutations in the MMACHC gene, which is located on chromosome 1p34.1 [1]

  • Since methylcobalamin is the essential cofactor for the enzyme methionine synthase, the defect causes an impairment of the remethylation of homocysteine (Hcy) to methionine (Met)

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Summary

Introduction

The cblC defect is a rare inborn error of intracellular cobalamin metabolism. The cblC defect (ORPHA 79282; MIM 277400) is an inborn error of intracellular cobalamin (cbl) metabolism caused by mutations in the MMACHC gene, which is located on chromosome 1p34.1 [1]. Since methylcobalamin is the essential cofactor for the enzyme methionine synthase, the defect causes an impairment of the remethylation of homocysteine (Hcy) to methionine (Met). Biochemical markers for the disease are elevated total Hcy (tHcy) in plasma and MMA in plasma and urine in the presence of low plasma Met concentrations. 90% of reported patients with the cblC defect present with the severe, infantile, early-onset form of the disease [3,4]. The true incidence of the late-onset cblC defect is probably higher than presently reported since in many cases the diagnosis may be missed

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