Pharmacokinetics and pharmacodynamics of anti-infective agents during continuous veno-venous hemofiltration in critically ill patients: Lessons learned from an ancillary study of the IVOIRE trial

Author:

Breilh Dominique1,Honore Patrick M.2,De Bels David2,Roberts Jason A.3,Gordien Jean Baptiste1,Fleureau Catherine4,Dewitte Antoine4,Coquin Julien4,Rozé Hadrien4,Perez Paul5,Attou Rachid2,Redant Sebastien2,Kugener Luc2,Saux Marie-Claude1,Spapen Herbert D.6,Ouattara Alexandre47,Joannes-Boyau Olivier4

Affiliation:

1. Laboratory of Clinical Pharmacokinetics and Clinical Pharmacy , INSERM U1034 , Haut-Lévêque Hospital, CHU Bordeaux , University of Bordeaux , Segalen, Pessac, France

2. Intensive Care Department , Centre Hospitalier Universitaire Brugmann-Brugmann University Hospital , Brussels , Belgium

3. University of Queensland Centre for Clinical Research , Faculty of Medicine & Centre for Translational Anti-infective Pharmacodynamics, School of Pharmacy , The University of Queensland , Brisbane , Australia

4. CHU Bordeaux , Department of Anaesthesia and Critical Care , Magellan Medico-Surgical Centre , F-33000 Bordeaux , France

5. Centre Hospitalier Universitaire de Bordeaux , Pôle de Santé Publique, Unité de Soutien Méthodologique à la Recherche Clinique et Épidémiologique , France

6. Ageing & Pathology Research Group , Vrije Universiteit Brussel , Brussels , Belgium

7. Biology of Cardiovascular Diseases, INSERM, UMR 1034 , University of Bordeaux , F-33600 Pessac, France

Abstract

Abstract Background Hemofiltration rate, changes in blood and ultrafiltration flow, and discrepancies between the prescribed and administered doses strongly influence pharmacokinetics (PK) and pharmacodynamics (PD) of antimicrobial agents during continuous veno-venous hemofiltration (CVVH) in critically ill patients. Methods Ancillary data were from the prospective multicenter IVOIRE (hIgh VOlume in Intensive caRE) study. High volume (HV, 70 mL/kg/h) was at random compared with standard volume (SV, 35 mL/kg/h) CVVH in septic shock patients with acute kidney injury (AKI). PK/PD parameters for all antimicrobial agents used in each patient were studied during five days. Results Antimicrobial treatment met efficacy targets for both percentage of time above the minimal inhibitory concentration and inhibitory quotient. A significant correlation was observed between the ultrafiltration flow and total systemic clearance (Spearman test: P < 0.005) and between CVVH clearance and drug elimination half-life (Spearman test: P < 0.005). All agents were easily filtered. Mean sieving coefficient ranged from 38.7% to 96.7%. Mean elimination half-life of all agents was significantly shorter during HV-CVVH (from 1.29 to 28.54 h) than during SV-CVVH (from 1.51 to 33.85 h) (P < 0.05). Conclusions This study confirms that CVVH influences the PK/PD behavior of most antimicrobial agents. Antimicrobial elimination was directly correlated with convection rate. Current antimicrobial dose recommendations will expose patients to underdosing and increase the risk for treatment failure and development of resistance. Dose recommendations are proposed for some major antibiotic and antifungal treatments in patients receiving at least 25 mL/kg/h CVVH.

Publisher

Walter de Gruyter GmbH

Subject

Internal Medicine

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