Mechanism of Microbial Transformation of Cholesterol into Coprostanol

Björkhem, Ingemar; Gustafsson, Jan‐Åke

doi:10.1111/j.1432-1033.1971.tb01488.x

Cited by 117 publications

(73 citation statements)

References 21 publications

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“…It is noteworthy that the sterol 27-hydroxylase is located at the inner membranes of the mitochondria (21). The nature of the mechanism behind transfer of cholesterol from the outer to the inner mitochondrial membranes in the present cells is not known.…”

Section: Elimination Of Cholesterol By Sterol 27-hydroxylase Mechanismmentioning

confidence: 92%

“…Two of the patients had a deletion of thymine in exon 4, and one had a splice junction mutation in intron 4 as described previously (11). The patients (20,21, and 15 years, respectively) had xanthomas and elevated serum cholestanol levels typical for the disease (12). Blood was drawn from these patients and from healthy volunteers for isolation of monocytes (see below).…”

Section: Methodsmentioning

confidence: 99%

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Elimination of Cholesterol in Macrophages and Endothelial Cells by the Sterol 27-Hydroxylase Mechanism

Babiker

Andersson

Lund

et al. 1997

Journal of Biological Chemistry

220

165

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Cultured macrophages and endothelial cells have been reported to secrete 27-oxygenated metabolites of cholesterol. This mechanism was compared with the classical high density lipoprotein (HDL)-dependent reverse cholesterol transport. Under standard conditions, macrophage preparations had considerably higher capacity to secrete 27-hydroxycholesterol and 3␤-hydroxy-5-cholestenoic acid than had endothelial cells and fibroblasts. Western blotting showed that lung macrophages contained the most sterol 27-hydroxylase protein of the cells tested. The relative amounts of 3␤-hydroxy-5-cholestenoic acid produced by the macrophages were also highest. Macrophages derived from monocytes of patients with sterol 27-hydroxylase deficiency did not secrete 27-oxygenated products, demonstrating that sterol 27-hydroxylase is the critical enzyme for the conversion of cholesterol into the 27-oxygenated steroids. That sterol 27-hydroxylase is responsible not only for 27-hydroxylation of cholesterol but also for the further oxidation of this steroid into 3␤-hydroxy-5-cholestenoic acid was shown with use of tritium-labeled 27-hydroxycholesterol and an inhibitor of sterol 27-hydroxylase.Secretion of 27-oxygenated products by the cultured macrophages as well as the ratio between the alcohol and the acid appeared to be dependent upon total 27-hydroxylase activity, the availability of substrate cholesterol, and the presence of an acceptor for 27-hydroxycholesterol in the medium. With albumin as extracellular acceptor, the major secreted product was 3␤-hydroxy-5-cholestenoic acid. Under such conditions, secretion of labeled 27-oxygenated products was higher than that of labeled cholesterol from lung alveolar macrophages preloaded with [4-14 C]cholesterol. With HDL as acceptor, 27-hydroxycholesterol was the major secreted product, and the total secretion of labeled 27-oxygenated products was only about 10% of that of labeled cholesterol. Thus, 27-hydroxycholesterol and cholesterol may compete for HDL-mediated efflux from the cells.The results support the contention that the sterol 27-hydroxylase-mediated elimination of cholesterol is more important in macrophages than in endothelial cells. This mechanism may be an alternative and/or a complement to the classical HDL-mediated reverse cholesterol transport in macrophages, in particular when the concentration of HDL is low.

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Section: Elimination Of Cholesterol By Sterol 27-hydroxylase Mechanismmentioning

confidence: 92%

Section: Methodsmentioning

confidence: 99%

Elimination of Cholesterol in Macrophages and Endothelial Cells by the Sterol 27-Hydroxylase Mechanism

Babiker

Andersson

Lund

et al. 1997

Journal of Biological Chemistry

220

165

View full text Add to dashboard Cite

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“…17 ) This mitochondrial hydroxylase requires NADPH generated by the NADP-dependent isocitrate dehydrogenase or by transhydrogenation of NADH formed during oxidation of organic acids in the citric acid cycle. 18) Therefore, it remains possible that succinyl CoA and its precursors caused an elevated production of bile acids via mitochondrial cholesterol 70:-hydroxylase. However, since additions of oxaloacetate and malate, which can easily penetrate into mitochondria, did not increase the bile acid secretion, the contribution of the mitochondrial 70:-hydroxylase to the bile acid synthesis appears to be small.…”

Section: Resultsmentioning

confidence: 99%

Propionate Enhances Synthesis and Secretion of Bile Acids in Primary Cultured Rat HepatocytesviaSuccinyl CoA

Imaizumi

Hirata

Yasni

et al. 1992

Bioscience, Biotechnology, and Biochemistry

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“…Thus the coprostanol formed from the mixture of 7a-3H-and 4-'4C-labeled cholesterol had the same 3H/'4C ratio as the precursor. Since the biosynthesis of coprostanol also involves 4-cholesten-3-one as an intermediate (29), an isotope effect in the conversion of cholesterol into 4-cholesten-3-one should have been reflected by a lowered 3H/ 14C ratio in coprostanol.…”

Section: Discussionmentioning

confidence: 99%

A novel pathway for biosynthesis of cholestanol with 7 alpha-hydroxylated C27-steroids as intermediates, and its importance for the accumulation of cholestanol in cerebrotendinous xanthomatosis.

Skrede¹,

Björkhem²,

Buchmann³

et al. 1985

J. Clin. Invest.

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A mixture of 7a-3H-and 4-'4C-labeled cholesterol was administered intravenously to rats. Cholestanol with 20-30% lower ratio between 3H and '4C than in cholesterol could be isolated from different organs. In a healthy human control, cholestanol isolated from feces had a 3H/'4C ratio which was 28% lower than in administered cholesterol. Cholesterol and coprostanol reisolated in these experiments had the same ratio between 3H and 14C as in the precursor. A previously unknown pathway for formation of cholestanol, involving 7a-hydroxylated intermediates, may explain these results. Under normal conditions, this pathway is responsible for at most 30% of the cholestanol synthesized from cholesterol.Intravenous administration of the 7a-3H-and 4-'4C-labeled cholesterol to a patient with cerebrotendinous xanthomatosis (CTX) resulted in formation of cholestanol which had 70-75% lower 3H/'4C ratio. It is concluded that the novel pathway involving 7a-hydroxylated intermediates is accelerated in patients with CTX. This acceleration may contribute essentially to the accumulation of cholestanol, which is a predominant feature of this disease.7a-Hydroxycholesterol and 7a-hydroxy4-cholesten-3-one might be intermediates in the novel pathway to cholestanol. After intravenous administration of 7_-3H-labeled 7a-hydroxycholesterol in a patient with CTX, significant amounts of 3H were incorporated into plasma and fecal cholestanol. Only small amounts of 7a-hydroxycholesterol and 7a-hydroxy-4-cholesten-3-one are excreted into the intestine, and we therefore conclude that the 7a-dehydroxylation step mainly occurs in the liver. In CTFX, the synthesis of cholestanol may be accelerated because the concentrations of 7a-hydroxylated bile acid intermediates in the liver are increased. A possible mechanism for the conversion of a minor fraction of 7a-hydroxycholesterol into cholestanol is suggested.

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Mechanism of Microbial Transformation of Cholesterol into Coprostanol

Cited by 117 publications

References 21 publications

Elimination of Cholesterol in Macrophages and Endothelial Cells by the Sterol 27-Hydroxylase Mechanism

Elimination of Cholesterol in Macrophages and Endothelial Cells by the Sterol 27-Hydroxylase Mechanism

Propionate Enhances Synthesis and Secretion of Bile Acids in Primary Cultured Rat HepatocytesviaSuccinyl CoA

A novel pathway for biosynthesis of cholestanol with 7 alpha-hydroxylated C27-steroids as intermediates, and its importance for the accumulation of cholestanol in cerebrotendinous xanthomatosis.

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