Ventilator-Associated Pneumonia Clinical Trial
Official title:
The Pharmacodynamics of Doripenem Between 4-hour and 1-hour Infusion in Patients With Ventilator-associated Pneumonia
This is prospective and randomized study to assess the pharmacodynamics (t>MIC) of 0.5 g
every 8 h of doripenem in patients with VAP following administration by a 4 h infusion or 1
h infusion.
Clinical and laboratory data such as Age,Sex, Body weight, Electrolyte, Vital signs, APACHE
II score, BUN, Cr, Blood culture will be collected.
Twelve patients will be enrolled in this study. After completion of the doripenem therapy
for 3 days in this study, all patients will receive other sensitive antibiotics to eradicate
their bacterial infections.
Doripenem pharmacokinetic study will be carried out during the doripenem therapy. Blood
samples (approximately 2 ml) in group " 0.5 g of doripenem with 4 h infusion every 8 h
regimen" will be obtained by direct venepuncture at the following time: 0, 0.5, 1, 2, 3, 4,
4.5, 5, 6, 7 and 8 h after 7th dose of doripenem.
Blood samples (approximately 2 ml) in group " 0.5 g of doripenem with 1 h infusion every 8 h
regimen" will be obtained by direct venepuncture at the following time: 1, 1.5, 2, 4, 5, 6,
7 and 8 h after 7th dose of doripenem.
The doripenem assays by method of Ikeda K et al. (J Chromatogr B, 2008) will be performed.
Concentration of doripenem in plasma will be simulated in Monte Carlo technique (Computer
model) to get PK/PD index (40%T>MIC) and reported to % PTA (Probability Target Attainment)
and %CFR (Cumulative Faction Response)
Introduction:
The treatment of resistant pathogens is becoming more difficult, and only a few novel
antimicrobial agents are currently in development with activity against highly resistant
Gram negative bacteria. Doripenem is a carbapenem antibacterial agent with a broad spectrum
of activity against Gram-negative and Gram-positive bacteria. This agent is often used as
the last line of therapy for highly resistant Gram negative bacilli nosocomial pathogens. In
common with other beta-lactam, the main pharmacokinetic/pharmacodynamic (PK/PD) index that
correlates with the therapeutic efficacy is the time that concentrations in the tissue and
serum are above the MIC (t>MIC). However, in tropical countries the stability of carbapenem
antibiotics is an important consideration when considering continuous infusion. Therefore,
prolonged infusion may be a useful route of administration to maximize bactericidal
activity. In addition, pharmacokinetic changes have been found for several antimicrobial
agents in critically ill patients, including ventilator-associated pneumonia. However, until
now we have had no data to reveal the PK/PD index of doripenem in these critically ill
patients.
Objectives:
To assess the pharmacodynamics (t>MIC) of 0.5 g every 8 h of doripenem in patients with VAP
following administration by a 4 h infusion or 1 h infusion.
Clinical and laboratory data: Age,Sex, Body weight, Electrolyte, Vital signs, APACHE II
score, BUN, Cr, Blood culture
Drug preparation and administration:
Doripenem will be reconstituted with saline solution according to the manufacturer's
guidelines and then administered to the patients by 2 regimens:
1.0.5 g in 100 ml of normal saline solution and administered via an infusion pump at a
constant flow rate over 4 h every 8 h.
2.0.5 g in 100 ml of normal saline solution and administered via an infusion pump at a
constant flow rate over 1 h every 8 h.
Study design:
The study is planned as a prospective and randomized in patients with VAP. Each patients
will receive doripenem in 2 regimens at room temperature (37°C) consecutively: (i) infusion
of 0.5 g of doripenem for 4 h via an infusion pump at a constant flow rate every 8 h; (ii)
infusion of 0.5 g of doripenem for 1 h via an infusion pump at a constant flow rate every 8
h.
Twelve patients will be enrolled in this study. After completion of the doripenem therapy
for 3 days in this study, all patients will receive other sensitive antibiotics to eradicate
their bacterial infections.
Sample collections:
Doripenem pharmacokinetic study will be carried out during the doripenem therapy.
Blood samples (approximately 2 ml) in group " 0.5 g of doripenem with 4 h infusion every 8 h
regimen" will be obtained by direct venepuncture at the following time: 0, 0.5, 1, 2, 3, 4,
4.5, 5, 6, 7 and 8 h after 7th dose of doripenem.
Blood samples (approximately 2 ml) in group " 0.5 g of doripenem with 1 h infusion every 8 h
regimen" will be obtained by direct venepuncture at the following time: 1, 1.5, 2, 4, 5, 6,
7 and 8 h after 7th dose of doripenem.
All blood samples will be allowed to clot and then cebtrifuged at 2,000g.
The serum obtained will be stored at-80°C until analysis.
Doripenem assay:
The doripenem assays by method of Ikeda K et al. (J Chromatogr B, 2008) will be performed at
Department of Medicine, Faculty of Medicine.
Clinical data and pathogens collection:
1. Initial patient demographic data (age, sex, weight, diagnosis, APACHE II scores) will
be collected upon enrollment in the study.
2. The Gram negative bacilli isolated from sputum in 12 patients will be collected and the
MIC of the doripenem for pathogens will be determined by E tests upon enrollment in the
study.
Duration of study:
Patients will receive doripenem for 3 days
Pharmacokinetic and pharmacodynamic analysis:
Concentration of doripenem in plasma will be simulated in Monte Carlo technique (Computer
model) to get PK/PD index (40%T>MIC) and reported to % PTA (Probability Target Attainment)
and %CFR (Cumulative Faction Response)
Sample Size: Twelve patients with VAP will be enrolled in this study.
;
Allocation: Randomized, Endpoint Classification: Pharmacokinetics/Dynamics Study, Intervention Model: Parallel Assignment, Masking: Open Label
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