IMPORTANCE OF PEROXISOMES IN THE FORMATION OF CHENODEOXYCHOLIC ACID IN HUMAN LIVER - METABOLISM OF 3-ALPHA, 7-ALPHA-DIHYDROXY-5-BETA-CHOLESTANOIC ACID IN ZELLWEGER SYNDROME

被引:12
作者
KASE, BF
PEDERSEN, JI
WATHNE, KO
GUSTAFSSON, J
BJORKHEM, I
机构
[1] UNIV OSLO,SCH MED,INST NUTR RES,OSLO 3,NORWAY
[2] CENT HOSP AKERSHUS,DEPT PEDIAT,AKERSHUS,NORWAY
[3] UNIV HOSP UPPSALA,DEPT PEDIAT,S-75185 UPPSALA,SWEDEN
[4] HUDDINGE UNIV HOSP,DEPT CLIN CHEM,S-14186 HUDDINGE,SWEDEN
来源
PEDIATRIC RESEARCH | 1991年 / 29卷 / 01期
关键词
D O I
10.1203/00006450-199101000-00013
中图分类号
R72 [儿科学];
学科分类号
100202 ;
摘要
Infantile Zellweger syndrome belongs to the group of peroxisomal disorders that lack peroxisomes. Both trihydroxycoprostanic acid (THCA), the precursor to cholic acid, and dihydroxycoprostanic acid (DHCA), the precursor to chenodeoxycholic acid, accumulate in this disease. In previous studies, we have shown that liver peroxisomes are required for the conversion of THCA into cholic acid both in vitro and in vivo by measuring a defective conversion in infants with Zellweger syndrome. In our present study, the conversion of DHCA into chenodeoxycholic acid has been measured in an infant with Zellweger syndrome to evaluate the importance of liver peroxisomes for the formation of chenodeoxycholic acid. Coprostanic acidemia was present from the second day of life with high levels of THCA and only trace amounts of DHCA. The conversion of i.v. administered [H-3]DHCA into chenodeoxycholic acid was only 7% compared with the 80% conversion in an analogous study in an adult. There was, however, a rapid incorporation of H-3 into biliary THCA and, after a lag phase, the H-3 was incorporated into biliary cholic acid. After 72 h, 15% of [H-3]DHCA was converted to cholic acid. The pool size of DHCA was 1.2 mg/m2 and the pool size of both cholic acid and chenodeoxycholic acid was markedly reduced. The renal excretion of cholic acid was more efficient than that of the less polar chenodeoxycholic acid. More polar metabolites of DHCA and THCA are formed in alternative metabolic pathways facilitating renal excretion of these toxic intermediates. We conclude that liver peroxisomes are essential for a normal conversion of DHCA into chenodeoxycholic acid.
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页码:64 / 69
页数:6
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