Abstract
Background: Molybdenum cofactor deficiency (MOCD) is a severe autosomal recessive neonatal metabolic disease that causes seizures and death or severe brain damage. Symptoms, signs and cerebral images can resemble those attributed to intrapartum hypoxia. In humans, molybdenum cofactor (MOCO) has been found to participate in four metabolic reactions: aldehyde dehydrogenase (or oxidase), xanthine oxidoreductase (or oxidase) and sulfite oxidase, and some of the components of molybdenum cofactor synthesis participate in amidoxime reductase. A newborn girl developed refractory seizures, opisthotonus, exaggerated startle reflexes and vomiting on the second day of life. Treatment included intravenous fluid, glucose supplementation, empiric antibiotic therapy and anticonvulsant medication. Her encephalopathy progressed, and she was given palliative care and died aged 1. week. There were no dysmorphic features, including ectopia lentis but ultrasonography revealed a thin corpus callosum. Objectives: The aim of this study is to provide etiology, prognosis and genetic counseling.
Original language | English |
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Pages (from-to) | 43-49 |
Number of pages | 7 |
Journal | Meta Gene |
Volume | 3 |
DOIs | |
Publication status | Published - 2015 |
Keywords
- genetic disorders
- metabolism
- molybdenum
- newborn infants
- pediatrics