We describe a metabolic defect in bile acid synthesis involving a deficiency in 7alpha-hydroxylation due to a mutation in the gene for the microsomal oxysterol 7alpha-hydroxylase enzyme, active in the acidic pathway for bile acid synthesis. The defect, identified in a 10-wk-old boy presenting with severe cholestasis, cirrhosis, and liver synthetic failure, was established by fast atom bombardment ionization-mass spectrometry, which revealed elevated urinary bile acid excretion, a mass spectrum with intense ions at m/z 453 and m/z 510 corresponding to sulfate and glycosulfate conjugates of unsaturated monohydroxy-cholenoic acids, and an absence of primary bile acids. Gas chromatography-mass spectrometric analysis confirmed the major products of hepatic synthesis to be 3beta-hydroxy-5-cholenoic and 3beta-hydroxy-5-cholestenoic acids, which accounted for 96% of the total serum bile acids. Levels of 27-hydroxycholesterol were > 4,500 times normal. The biochemical findings were consistent with a deficiency in 7alpha-hydroxylation, leading to the accumulation of hepatotoxic unsaturated monohydroxy bile acids. Hepatic microsomal oxysterol 7alpha-hydroxylase activity was undetectable in the patient. Gene analysis revealed a cytosine to thymidine transition mutation in exon 5 that converts an arginine codon at position 388 to a stop codon. The truncated protein was inactive when expressed in 293 cells. These findings indicate the quantitative importance of the acidic pathway in early life in humans and define a further inborn error in bile acid synthesis as a metabolic cause of severe cholestatic liver disease.
K D Setchell, M Schwarz, N C O'Connell, E G Lund, D L Davis, R Lathe, H R Thompson, R Weslie Tyson, R J Sokol, D W Russell
Title and authors | Publication | Year |
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Journal of Clinical Investigation | 2000 |
THEROLE OFORPHANNUCLEARRECEPTORS IN THEREGULATION OFCHOLESTEROLHOMEOSTASIS
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Annual Review of Cell and Developmental Biology | 2000 |
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Gut | 2000 |
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P Honkakoski, M Negishi |
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R Morfin, P Lafaye, AC Cotillon, F Nato, V Chmielewski, D Pompon |
Annals of the New York Academy of Sciences | 2000 |
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R Poupon, O Chazouillères, RE Poupon |
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WF Balistreri |
Clinics in Liver Disease | 2000 |
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KE Bove |
Clinics in Liver Disease | 2000 |
The NAD+ precursors, nicotinic acid and nicotinamide protect cells against apoptosis induced by a multiple stress inducer, deoxycholate
CL Crowley, CM Payne, H Bernstein, C Bernstein, D Roe |
Cell Death and Differentiation | 2000 |
Disruption of the Oxysterol 7α-Hydroxylase Gene in Mice
J Li-Hawkins, EG Lund, SD Turley, DW Russell |
The Journal of biological chemistry | 2000 |
Oxysterol 7α-Hydroxylase Activity by Cholesterol 7α-Hydroxylase (CYP7A)
M Norlin, U Andersson, I Björkhem, K Wikvall |
The Journal of biological chemistry | 2000 |
Expression Cloning of an Oxysterol 7α-Hydroxylase Selective for 24-Hydroxycholesterol
J Li-Hawkins, EG Lund, AD Bronson, DW Russell |
The Journal of biological chemistry | 2000 |
Kinetics and plasma concentrations of 26-hydroxycholesterol in baboons
S Li, J Pang, EM Jackson, WK Wilson, GE Mott, GJ Schroepfer |
Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids | 2000 |
Cholestenoic Acid Is a Naturally Occurring Ligand for Liver X Receptor α**This work was supported by NIH grants
C Song, S Liao |
Endocrinology | 2000 |
Plasma levels of 24S-hydroxycholesterol reflect the balance between cerebral production and hepatic metabolism and are inversely related to body surface
L Bretillon, D Lütjohann, L Ståhle, T Widhe, L Bindl, G Eggertsen, U Diczfalusy, I Björkhem |
Journal of lipid research | 2000 |