Influence of body temperature on indinavir crystallization under loop of Henle conditions

doi:10.1093/jac/dkl436

JAC Advance Access originally published online on November 9, 2006
Journal of Antimicrobial Chemotherapy 2007 59(1):114-117; doi:10.1093/jac/dkl436

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© The Author 2006. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved. For Permissions, please e-mail: journals.permissions@oxfordjournals.org

Influence of body temperature on indinavir crystallization under loop of Henle conditions

Saima Salahuddin¹^,2, Dik J. Kok¹ and Noor N.-P. Buchholz²^,*

¹ Department of Experimental Urology, Erasmus Medical Centre Dr Molenwaterplein, 3010 GD, Rotterdam, The Netherlands ² Department of Urology, St Bartholomew's Hospital Barts and The London NHS Trust, London EC1A 7BE, UK

Received 1 July 2006; returned 10 August 2006; revised 1 October 2006; accepted 4 October 2006

^*Corresponding author. Tel: +44-207-6018394; Fax: +44-207-6017844; E-mail: nielspeter{at}yahoo.com

Objectives: Indinavir is a protease inhibitor used in the therapyof HIV-1+ patients. It causes indinavir stone formation. Ithas been shown to precipitate in the loop of Henle (LH) at plasmaconcentrations (conc[P]) of $~$ 8 mg/L. Those experiments were performedat room temperature. Given the influence of temperature on crystallizationin general, and solubility of indinavir in particular, we repeatedthe experiments under physiological (body) temperature conditions.

Methods: Test solutions contained indinavir concentrations of100–750 mg/L at ionic strengths varying from 0 to 800mM simulating conditions in the proximal tubule and the LH.Solutions were titrated with base (NaOH) to find the pH valuewhere nucleation is initiated. Experiments were conducted atroom temperature (20°C) and repeated under constantly monitored(body) temperature (37°C).

Results: Experiments at 20°C confirmed our previous results.At 37°C, the relationship between pH and indinavir concentrationremained inversely proportional. Again, the LH was confirmedas the most likely localization of crystallization. However,at 37°C precipitation occurred at a lower urinary concentration(100 versus 125 mg/L) and within a lower pH range (6.67–7.26versus 7.23–7.44). This lower urinary concentration correspondsto a lower conc[P] [critical value (CV)] of 6.41 mg/L, as comparedwith 8.01 mg/L at 20°C.

Conclusions: The CV is even lower at 37°C than previouslyassumed. Plasma peak concentration above the CV of 6.4 mg/Lwill induce crystallization in the LH and should be avoided.

Keywords: protease inhibitors , drug kinetics , dosages , in vitro experiments

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