Pharmacokinetics and Antidepressant Activity of Fluoxetine in Transgenic Mice with Elevated Serum Alpha-1-Acid Glycoprotein Levels

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Vol. 26, Issue 1, 20-24, January 1998

Pharmacokinetics and Antidepressant Activity of Fluoxetine in Transgenic Mice with Elevated Serum Alpha-1-Acid Glycoprotein Levels

John W. Holladay, Michael J. Dewey and Sun D. Yoo

College of Pharmacy (J.W.H.) and the Department of Biological Sciences, College of Science and Mathematics (M.J.D.), University of South Carolina and the College of Pharmacy, SungKyunKwan University (S.D.Y.)

Fluoxetine, a novel selective serotonin reuptake inhibitor utilized in the treatment of depression, is avidly bound to serumalbumin and alpha-1-acid glycoprotein (AAG). AAG is an acute phaseprotein, and its serum levels are elevated in a variety of pathophysiologicalconditions including inflammation, depression, cancer, and acquiredautoimmune deficiency syndrome. Further, the pharmacokinetic dispositionand pharmacological activity of several highly bound drugs havebeen reported to be significantly altered as a result of elevatedserum AAG. We investigated the effects of elevated serum AAG levelson the pharmacokinetic disposition, antidepressant activity, andsteady state profile of fluoxetine and its demethylated metabolite,norfluoxetine. This was approached utilizing a novel strain oftransgenic mice that expressed genetically elevated serum AAGlevels severalfold over those of control mice. Serum and braindrug concentrations were determined by HPLC after fluoxetine administration.In transgenic mice, the volume of distribution and the terminalelimination half-life of fluoxetine were significantly reduced.Further, significant reductions in brain-to-serum fluoxetine concentrationratios and antidepressant activity were observed in transgenicmice, despite having higher serum drug levels than control mice.This trend in the serum continued at steady state, and brain fluoxetinelevels were significantly lower in transgenic mice. The resultsof this study provide valuable insights regarding the consequencesof elevated serum AAG levels, often seen in several disease states,on the pharmacokinetic disposition of fluoxetine.

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