1.A Case of Rhizomelic Chondrodysplasia Punctata Type I.
Dal Hyun KIM ; Young Se KWON ; Yong Hoon JUN ; Young Jin HONG ; Byoung Kwan SON ; Hye Ran YOON
Journal of the Korean Pediatric Society 2002;45(12):1585-1590
Rhizomelic chondrodysplasia punctata(RCDP) is a rare autosomal recessive disorder clinically characterized by symmetrical shortening of the proximal limbs, contractures of joints, a typical dysmorphic face, cataracts, and itchyosis. Patients with RCDP can be subdivided into three subgroups based on biochemical analysis and complementation studies. RCDP type I results from mutations in the PEX7 gene encoding the peroxisomal targeting signal type II(PST2) receptors and presents with both a defect in plasmalogen biosynthesis and phytanic acid oxidation. RCDP type II is deficient in the activity of dihydroxyacetonephosphate acyltransferase(DHAP-AT). RCDP type III is deficient in alkyl-dihydroxyacetonephosphate synthase(alkyl-DHAP). We report a case of RCDP type I which was confirmed with biochemical study, fibroblast culture, and gene study.
Cataract
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Chondrodysplasia Punctata, Rhizomelic*
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Complement System Proteins
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Contracture
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Extremities
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Fibroblasts
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Humans
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Joints
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Phytanic Acid
2.A Case of Neonatal Adrenoleukodystrophy Presented with Neonatal Seizure.
Jungi CHOI ; Su Jeong YOU ; Tae Sung KO ; Ellen Ai Rhan KIM ; Ki Soo KIM ; Soo Young PI ; Han Wook YOO
Journal of the Korean Child Neurology Society 2005;13(1):99-103
Neonatal adrenoleukodystrophy(NALD) is an inherited autosomal recessive disease characterized by very early onset of neurologic deterioration, extreme hypotonia, poor sucking reflex, failure to thrive, poor or absent grasp and Moro reflexes, diminished deep tendon reflexes, neonatal seizure refractory to antiepileptic drugs, progressive hepatomegaly, and mild or absent craniofacial dysmorphism. In the peroxisomal biogenesis disorders, whose basic defect are the incapabilities to import one or more proteins into the organelle, include Zellweger syndrome(ZS), NALD, and infantile Refsum disease(IRD). These are now thought to represent a continuous spectrum of disease severity, ZS the most severe, IRD the least severe, and NALD intermediate. Furthermore, their biochemistry and microscopic pathology are nearly identical. The biochemical abnormalities of NALD are the elevated levels of very long chain fatty acid(VLCFA), phytanic acid, pristanic acid, pipecolic acid in plasma, cultured skin fibroblasts, and reduced plasmalogen contents in erythrocytes. There are no effective treatments until now. We experienced an one day old neonate with hypotonia and seizure, who was diagnosed as NALD by elevated plasma VLCFA. So we report the case with a brief review of literature.
Anticonvulsants
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Biochemistry
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Organelle Biogenesis
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Erythrocytes
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Failure to Thrive
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Fibroblasts
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Hand Strength
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Hepatomegaly
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Humans
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Infant, Newborn
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Muscle Hypotonia
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Organelles
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Pathology
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Peroxisomal Disorders*
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Phytanic Acid
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Plasma
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Reflex
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Reflex, Stretch
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Seizures*
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Skin