Abstract
GRACILE syndrome belongs to the Finnish disease heritage, and is caused by a point mutation in the BCS1L-gene encoding a mitochondrial protein. This leads to dysfunction of the complex III in the respiratory chain. Significant fetal growth disturbance is the primary manifestation. Within the first day the newborn infant develops severe lactic acidosis. Hypoglycemia, elevated serum ferritin and conjugated bilirubin values and aminoaciduria imply mitochondrial liver disease and renal tubulopathy. In Finland, the diagnosis is based on the 232A>G mutation in the BCS1L-gene. No specific treatment is available. GRACILE syndrome leads to early death.
MeSH terms
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ATPases Associated with Diverse Cellular Activities
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Acidosis, Lactic / diagnosis*
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Acidosis, Lactic / epidemiology
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Acidosis, Lactic / genetics
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Biomarkers / blood
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Cholestasis / diagnosis*
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Cholestasis / epidemiology
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Cholestasis / genetics
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Electron Transport Complex III / genetics
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Fetal Growth Retardation / diagnosis*
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Fetal Growth Retardation / epidemiology
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Fetal Growth Retardation / genetics
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Finland / epidemiology
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Hemosiderosis / diagnosis*
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Hemosiderosis / epidemiology
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Hemosiderosis / genetics
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Humans
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Infant, Newborn
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Metabolism, Inborn Errors / diagnosis*
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Metabolism, Inborn Errors / epidemiology
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Metabolism, Inborn Errors / genetics
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Mitochondrial Diseases / congenital
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Point Mutation
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Renal Aminoacidurias / diagnosis*
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Renal Aminoacidurias / epidemiology
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Renal Aminoacidurias / genetics
Substances
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BCS1L protein, human
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Biomarkers
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ATPases Associated with Diverse Cellular Activities
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Electron Transport Complex III
Supplementary concepts
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Finnish lethal neonatal metabolic syndrome