Platelet-leucocyte adhesion markers before and after the initiation of antiretroviral therapy with HIV protease inhibitors

doi:10.1093/jac/dkn333

JAC Advance Access published online on August 27, 2008
Journal of Antimicrobial Chemotherapy, doi:10.1093/jac/dkn333

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© The Author 2008. 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

Original research

Platelet–leucocyte adhesion markers before and after the initiation of antiretroviral therapy with HIV protease inhibitors

Nils von Hentig¹^,*, Ann-Kristin Förster¹, Karina Kuczka¹, Ute Klinkhardt¹, Stefan Klauke², Peter Gute², Schlomo Staszewski³, Sebastian Harder¹ and Jochen Graff¹

¹ Pharmazentrum Frankfurt, Institute of Clinical Pharmacology, Johann Wolfgang Goethe University, Frankfurt, Germany ² Infektiologikum Frankfurt, Frankfurt, Germany ³ HIVCENTER, Medical HIV Treatment and Research Unit, Johann Wolfgang Goethe University, Frankfurt, Germany

Received 9 June 2008; returned 6 July 2008; revised 18 July 2008; accepted 19 July 2008

^* Corresponding author. Tel: +49-69-63016956; Fax: +49-69-63017636; E-mail: hentig{at}em.uni-frankfurt.de

Introduction: Thromboembolic complications under antiretroviral therapy (ART)have been described in the past. In particular, the influenceof protease inhibitors (PIs) on platelet activation and coagulationis currently under discussion.

Methods: HIV-1-infected, PI-naive adults (n = 18) were investigated beforeand 4 weeks after the start of the ART, consisting either ofboosted PI regimens (n = 13) plus reverse transcriptase inhibitors(RTIs) or a double PI regimen (n = 5) without RTI co-medication.Administered PIs were saquinavir (n = 15), lopinavir (n = 4),fosamprenavir (n = 2) and atazanavir (n = 2). Platelet CD62P,CD40L (%+ cells) and PAC-1 binding [mean fluorescence intensity(MFI)] as well as monocyte CD11b (MFI) and monocyte-associatedCD41 (%+ cells and MFI) expression were assessed by flow cytometrywith or without platelet stimulation. To investigate the influenceof platelets on coagulation, the endogenous thrombin potential(ETP) [render fluorescence units (RFI)] was determined.

Results: CD62P, PAC-1 binding and CD11b expression remained unchanged.In contrast, the mean±SD MFI of CD40L (from 18.2±9.0to 25.5±10.4, P = 0.038) and CD41 (from 446.1±213.8to 605.0±183.8, P = 0.010) as markers for increased platelet–leucocyteinteraction increased significantly. The collagen-induced ETPtime-to-peak was altered significantly from 23.8±11.4to 17.0±4.2 min (P = 0.028), although the ETP RFI peakshowed no evidence for increased procoagulatory capacity (47.1±18.6to 57.3±19.9, P = 0.085).

Conclusions: Effects of the evaluated PI HIV therapy on platelet functionassessed under field conditions seem to be minor, not affectingall investigated parameters. We found no evidence for increasedplatelet activation under PI-containing ART. However, CD41 asa marker for increased platelet–leucocyte interactionand CD40L, which can contribute to atherosclerosis, increasedsignificantly.

Key Words: HIV PIs , platelets , leucocytes , CD40L , CD41

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