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The Nature of the Copper Complexes in Bile and Their Relationship to the Absorption and Excretion of Copper in Normal Subjects and in Wilson's Disease

Overview
Journal Gut
Specialty Gastroenterology
Date 1973 Mar 1
PMID 4700437
Citations 7
Authors
K O Lewis
Affiliations
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Abstract

Copper in bile has been shown by electrophoresis to occur neither as free ions nor complexed to protein but to be associated with a component of the micellar complexes of bile. Solvent fractionation studies suggest that the bile salt components of the lecithin-bile salt complexes are the active binding agents. The effects of specific bile salts on the behaviour of copper during electrophoresis supports this possibility. The relationship of certain bile salts to the excretion of copper in man during the time that an external biliary fistula was functioning and to the intestinal absorption of copper in the rat was found to confirm this concept. The results show that copper in bile is associated with taurochenodeoxycholate and suggest an explanation for the elevated tissue copper levels found in Wilson's disease.

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References
1.
OWEN Jr C . ABSORPTION AND EXCRETION OF CU64-LABELED COPPER BY THE RAT. Am J Physiol. 1964; 207:1203-6. DOI: 10.1152/ajplegacy.1964.207.6.1203. View
2.
Weinbren K, Billing B . Hepatic clearance of bilirubin as an index of cellular function in the regenerating rat liver. Br J Exp Pathol. 1956; 37(2):199-204. PMC: 2082559. View
3.
Wheeler H, Ramos O . DETERMINANTS OF THE FLOW AND COMPOSITION OF BILE IN THE UNANESTHETIZED DOG DURING CONSTANT INFUSIONS OF SODIUM TAUROCHOLATE. J Clin Invest. 1960; 39(1):161-70. PMC: 290674. DOI: 10.1172/JCI104015. View
4.
Bergeret B, Chatagner F . [Enzymatic desulfination and decarboxylation of the l-cysteine sulfinic acid; its quantitative transformation into alanine & hypotaurine]. Biochim Biophys Acta. 1952; 9(2):141-6. DOI: 10.1016/0006-3002(52)90139-x. View
5.
Frommer D . The binding of copper by bile and serum. Clin Sci. 1971; 41(6):485-93. DOI: 10.1042/cs0410485. View