Jan Neal Hamilton scite author profile

Jan Neal Hamilton

3Publications

35Citation Statements Received

39Citation Statements Given

How they've been cited

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Affiliations

University of Minnesota Medical Center, Karolinska Institutet, United States Department of Veterans Affairs

Publications

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Bile acid synthesis in man. In vivo activity of the 25-hydroxylation pathway.

Duane¹,

Pooler²,

Hamilton³

1988

J. Clin. Invest.

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During biosynthesis of bile acid, carbons 25-26-27 are removed from the cholesterol side-chain. Side-chain oxidation begins either with hydroxylation at the 26-position, in which case the three-carbon fragment is released as propionic acid, or with hydroxylation at the 25-position, in which case the threecarbon fragment is released as acetone. We have previously shown in the rat that the contribution of the 25-hydroxylation pathway can be quantitated in vivo by measuring production of

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Quantitative importance of the 25-hydroxylation pathway for bile acid biosynthesis in the rat

Duane

Björkhem

Hamilton

et al. 1988

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During biosynthesis of bile acid, carbons 25-26-27 are removed from the cholesterol side chain. Side-chain oxidation begins either with hydroxylation at the 26-position, in which case the three-carbon fragment is released as propionic acid, or with hydroxylation at the 25-position, in which case the three-carbon fragment is released as acetone. In the present study, we have quantitated the relative importance of these two pathways in vivo by measuring production of [14C] acetone from [14C]-26-cholesterol. Four days after intraperitoneal injection of 20 to 40 muCi [14C]-26-cholesterol and 1 day after beginning a constant intravenous infusion of unlabeled acetone at 25 mumoles per kg per min, 6 male and 2 female Sprague-Dawley rats underwent breath collections. Expired acetone was trapped and purified as the 2,4-dinitrophenylhydrazine derivative. 14CO2 was trapped quantitatively using phenethylamine. Specific activity of breath acetone was multiplied times the acetone infusion rate to calculate production of [14C]acetone. [14C] Acetone production averaged 1.7% of total release of 14C from [14C]-26-cholesterol, estimated by 14CO2 output. The method was validated by showing that [14C] acetone production from [14C]isopropanol averaged 111% of the [14C]isopropanol infusion rate. We conclude that, in the normal rat, the 25-hydroxylation pathway accounts for less than 2% of bile acid synthesis.

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Studies of feedback suppression of bile salt synthesis in the bile-fistula rat.

Duane

McHale

Hamilton

1988

Journal of Lipid Research

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