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A NEW-TYPE OF DEFECT IN THE GENE FOR BILIRUBIN URIDINE 5'-DIPHOSPHATE-GLUCURONOSYLTRANSFERASE IN A PATIENT WITH CRIGIER-NAJJAR SYNDROME TYPE-I

被引:63
作者
AONO, S
YAMADA, Y
KEINO, H
SASAOKA, Y
NAKAGAWA, T
ONISHI, S
MIMURA, S
KOIWAI, O
SATO, H
机构
[1] AICHI PREFECTURAL COLONY,INST DEV RES,DEPT PERINATOL,KASUGAI,AICHI 48003,JAPAN
[2] OKAZAKI MUNICIPAL HOSP,DEPT PEDIAT,OKAZAKI,AICHI 444,JAPAN
[3] KAGAWA MED SCH,DEPT PEDIAT,KAGAWA 76107,JAPAN
[4] NAGOYA UNIV,SCH MED,DEPT PEDIAT,NAGOYA,AICHI 466,JAPAN
[5] AICHI CANC CTR,RES INST,DEPT BIOCHEM,NAGOYA,AICHI 464,JAPAN
[6] SHIGA UNIV MED SCI,DEPT BIOL,OTSU,SHIGA 52021,JAPAN
来源
PEDIATRIC RESEARCH | 1994年 / 35卷 / 06期
关键词
D O I
10.1203/00006450-199406000-00002
中图分类号
R72 [儿科学];
学科分类号
100202 [儿科学];
摘要
Crigler-Najjar syndrome (CN) type I, which is characterized by the complete absence of bilirubin uridine 5'-diphosphate-glucuronosyltransferase (UGT) activity, is inherited as an autosomal recessive trait associated with unconjugated hyperbilirubinemia. Phenobarbital has no effect on the bilirubin concentration in the serum of patients with CN type I. Recently, cDNA for two human liver bilirubin UGT (UGT1A and UGT1D) were isolated, and their genetic organization was determined. The UGT1A (UGT1*1) and UGT1D (UGT1*4) genes each have a unique exon 1, whereas exons 2-5 are common to both genes. It has been predicted that some defect in the exons common to both genes is responsible for the absence of UGT1A and UGT1D activities in CN type I, and five cases with such a mutation have been reported. We describe here a new type of defect in the gene for bilirubin UGT in a patient with CN type I, namely, an abnormality in the exon 1 that is characteristic of the UGT1A gene. This mutation is a single nucleotide substitution, that is, C is changed to A at base position 840 in UGT1A. cDNA, and this change results in a stop codon. Our patient is homozygous for the defect, and his nonconsanguineous parents and elder brother, who are clinically normal, are heterozygous for the defective allele. No mutation was detected in any exons of the UGT1D gene. Our results suggest that a homozygous nonsense or deletion mutation is detected not only in the exons common to UGT1A and UGT1D genes but also in unique exon 1 of UGT1A in CN type I.
引用
收藏
页码:629 / 632
页数:4
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