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Research Article

Hepatic Activation and Inactivation of Clinically-relevant Vitamin D Analogs and Prodrugs

GLENVILLE JONES, VALARIE BYFORD, SHELLY WEST, SONOKO MASUDA, GEORGE IBRAHIM, MARTIN KAUFMANN, JOYCE C KNUTSON, STEPHEN STRUGNELL and RAJENDRA MEHTA
Anticancer Research July 2006, 26 (4A) 2589-2595;
GLENVILLE JONES
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  • For correspondence: gj1{at}post.queensu.ca
VALARIE BYFORD
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SHELLY WEST
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SONOKO MASUDA
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GEORGE IBRAHIM
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MARTIN KAUFMANN
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JOYCE C KNUTSON
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STEPHEN STRUGNELL
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RAJENDRA MEHTA
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Abstract

Like most pharmaceutical agents, vitamin D analogs are subject to hepatic metabolism by a variety of cytochrome P450 (CYP)-based systems. Metabolism can involve activation as well as inactivation of the vitamin D analog and one of the more successful families includes the 1α-hydroxyvitamin D prodrugs (1α-OH-D2,1α-OH-D3,1α-OH-D4,1α-OH-D5), that all require a step of activation. Some of these prodrugs are in use or clinical trial because they have a therapeutic advantage over calcitriol. However, the nature of the activation of these molecules is poorly understood, particularly with regard to the CYP isoform involved. Various transfected CYPs and hepatic cell lines combined with tandem LC-MS analysis were used to investigate the metabolism of a spectrum of vitamin D analogs, including 1α-OH-Ds and the topical analog, calcipotriol. In the case of the 1α-OH-Ds, evidence was found of multiple sites of side-chain hydroxylation consistent with the generation of more than one active form. The potential involvement of CYP27A and other putative 25-hydroxylases in 1α-OH-D activation was also shown, as well as the potential for CYP24 activation and inactivation. In the case of calcipotriol, the respective roles of non-vitamin D-related CYPs and CYP24 in the catabolism of this anti-psoriatic drug were dissected out using cell lines with or without CYP24 expression, allowing us to demonstrate the potential contribution of CYP24 to “vitamin D resistance”. The implications of hepatic metabolism in the context of other facets thought to play a role in the mechanism of action of anticancer and antiproliferative vitamin D analogs are discussed.

  • Vitamin D analogs and prodrugs
  • hepatic activation
  • calcitriol
  • CYP

Footnotes

  • Received December 29, 2005.
  • Accepted January 9, 2006.
  • Copyright© 2006 International Institute of Anticancer Research (Dr. John G. Delinassios), All rights reserved
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Anticancer Research
Vol. 26, Issue 4A
July-August 2006
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Hepatic Activation and Inactivation of Clinically-relevant Vitamin D Analogs and Prodrugs
GLENVILLE JONES, VALARIE BYFORD, SHELLY WEST, SONOKO MASUDA, GEORGE IBRAHIM, MARTIN KAUFMANN, JOYCE C KNUTSON, STEPHEN STRUGNELL, RAJENDRA MEHTA
Anticancer Research Jul 2006, 26 (4A) 2589-2595;

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Hepatic Activation and Inactivation of Clinically-relevant Vitamin D Analogs and Prodrugs
GLENVILLE JONES, VALARIE BYFORD, SHELLY WEST, SONOKO MASUDA, GEORGE IBRAHIM, MARTIN KAUFMANN, JOYCE C KNUTSON, STEPHEN STRUGNELL, RAJENDRA MEHTA
Anticancer Research Jul 2006, 26 (4A) 2589-2595;
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