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Journal of Lipid Research, Vol 36, 1697-1707, Copyright © 1995 by Lipid Research, Inc.
CN van der Veere, B Schoemaker, R van der Meer, AK Groen, PL Jansen and RP Oude Elferink
The association of unconjugated bilirubin (UCB) with amorphous calcium
phosphate was studied in vitro. To this end UCB, solubilized in different
micellar bile salt solutions, was incubated with freshly prepared calcium
phosphate precipitate. It was demonstrated that amorphous calcium phosphate
(ACP) rapidly binds and precipitates UCB in a dose-dependent way. The
results indicate that binding of UCB to ACP is specific: binding to barium
phosphate was negligible and addition of low amounts of Mg2+ before
formation of the calcium phosphate precipitate (Ca:Mg = 5:1) inhibited
binding by 80%. Free Ca2+ stimulated binding, whereas free phosphate ions
inhibited binding of UCB in taurocholate solutions and to a lesser extent
in glycocholate solutions. The apparent affinity of UCB for amorphous
calcium phosphate was different in the various bile salt solutions. Binding
of UCB decreased at pH > 8.5 in taurocholate solutions, but not in
glycocholate solutions where binding of UCB was constant from pH 7.5- 10.5.
We propose a model in which UCB directly binds to amorphous calcium
phosphate in the presence of bile salts that weakly interact with ACP, like
taurocholate. In the presence of bile salts that strongly interact with
ACP, such as glycochenodeoxycholate, binding of UCB may also occur via the
bile salt. In conditions of unconjugated hyperbilirubinemia, such as the
Crigler-Najjar syndrome, neonatal jaundice, and in the Gunn rat,
considerable amounts of UCB diffuse across the intestinal mucosa. Binding
of UCB to calcium phosphate in the intestine may stimulate its excretion
and thereby constitute a relevant mechanism of excretion.
ARTICLES
Rapid association of unconjugated bilirubin with amorphous calcium phosphate
Department of Gastroenterology, Academic Medical Center, Amsterdam, The Netherlands.
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