Evaluation of Pharmacokinetic / Pharmacodynamic Data and Interest Individualized Therapeutic Drug Monitoring Glycopeptides and β-lactam-aminoglycoside ICU

Sponsor
Groupe Hospitalier Paris Saint Joseph (Other)
Overall Status
Active, not recruiting
CT.gov ID
NCT02846298
Collaborator
(none)
172
1
85.7
2

Study Details

Study Description

Brief Summary

Since the discovery of streptomycin in 1944, aminoglycosides retain a remarkable bactericidal activity vis-à-vis including aerobic gram-negative bacilli. Thus, their synergistic effect with beta-lactams and their rapid bactericidal on many make unavoidable pathogens and make it a cornerstone of the treatment of patients with severe sepsis or state of septic shock.

This is antibiotics exclusively parenteral administration. Their effectiveness is concentration-dependent and are administered by 30-minute infusion. Tolerance of venous is usually excellent. Their potential nephrotoxicity or cochleovestibular toxicity requires accurate monitoring of antibiotic residuals.

Moreover the fact that the effectiveness of the aminoglycosides is concentration dependent, the rate at the peak is decisive. A first sub-therapeutic dose leads to adaptively resistant bacteria compared to the aminoglycoside and therefore an increase of Minimal Inhibitory Concentrations (MIC). Many studies have been conducted in patients hospitalized in intensive care, highlighting underdoses in aminoglycosides when the prescribed dosages consistent with those used in non reanimated patients. Dr Moore showed in 89 ICU patients with bacteremia gram-negative bacilli, the relationship between the clinical course and obtaining whether therapeutic levels during the first administration of aminoglycosides. Thus, mortality in patients whose antibiotic concentrations to peak were subtherapeutic, amounted to 20.9% against 2.4% when concentrations were within the therapeutic range. In the context or an initial peak in the PK / PD ( Pharmacokinetic / Pharmacodynamic) objectives namely Cmax / MIC ≥ 8-10 desirable, individualized therapeutic drug monitoring and identification of factors that may cause a concentration of antibiotic at sub-therapeutic peak seems necessary , in patients for the majority an increased volume of distribution.

In addition to the β-lactams and glycopeptides, due to the increased volume of distribution in critically ill patients in sepsis, evaluation of serum 24 hours after starting treatment to check that the PK / PD goals for these molecules is achieved.

Condition or Disease Intervention/Treatment Phase
  • Biological: Drug Monitoring

Detailed Description

Primary / secondary objective

Investigators propose to conduct a study with the goal:
  • Evaluate the rate of patients for whom efficacy endpoint PK / PD Cmax / MIC ≥ 8-10 is reached at the first dose of the usual doses.

  • Compare the 30-day mortality among patients with subclinical a first rate versus those who have reached the desired peak

  • Evaluate the rate of patients for whom PK / PD efficiency target for related antibiotics is reached:

  • Serum residual> 4X MIC for the β-lactam rate and continuous function of β-lactam and the germ.

  • Serum between 25 and 35 mg / L vancomycin continuously.

  • Assess the factors associated with obtaining a rate of aminoglycoside subtherapeutic peak in a population of critically ill patients.

  • Assess the residual to 12h after injection to an anticipation of residual dosed at 24.

Methodology :
  • Type Of study:

  • Prospective, single-center type of professional practice evaluation

  • Expected duration of the study six months

  • Objective inclusion: 50 to 100 patients. Computing the number of patients to be included was done via the BioStaTGV software.

  • Description Of the study (according to recommendations):

  • Admission of patients in intensive care unit

  • Levy peak aminoglycoside 30min after the end of the 30 minutes of infusion the first administration

  • Collection of residual aminoglycoside to + 12h and between 23h-30 and 24 hours after injection.

  • Extraction of the residual H + 24h, 30 min before injection to the β-lactam associated administered discontinuously or without time constraints if administration batchwise to the β-lactam and vancomycin.

  • Routing unsettled and not frozen tubes in <2 hours of collection

  • Reception and registration levy of the laboratory assay of anti-infective under his usual care as recommended service

  • Determination of aminoglycoside and vancomycin immunoturbidimetric method (Indiko PLUS)

  • Β-lactam assay by LC-MS

  • Rendering the usual result (result server consultation for partial and report PDF available on the patient's medical record DXcare).

  • Director-post of MIC of aminoglycoside and β-lactam vis-à-vis the offending germ for each bacterial strain isolated and documenting infection

  • Destruction Levies: levies will not be retained after being used for the study. They will be destroyed in accordance with the rules of good practice research laboratories.

Data Monitoring and support:

Patient data will be collected on a computer CRF including clinical, biological and microbiological data of patients via the patient's medical record on DXcare: demographics, weight, height, BMI, hydration status, kidney function, liver function, shock, chronic heart failure, malnutrition, hypoalbuminemia burned, cirrhosis, chronic rheumatic disease, other antecedents, pregnancy, reason for hospitalization, etiology of sepsis motivating the introduction of aminoglycosides, β-lactam or glycopeptide and also other associated treatments. The data collected will help identify risk factors associated with a sub-therapeutic dosing aminoglycosides, β-lactam or glycopeptide.

Study Design

Study Type:
Observational
Actual Enrollment :
172 participants
Observational Model:
Cohort
Time Perspective:
Prospective
Official Title:
Evaluation of Pharmacokinetic / Pharmacodynamic Data and Interest Individualized Therapeutic Drug Monitoring Glycopeptides and β-lactam-aminoglycoside ICU
Actual Study Start Date :
Nov 8, 2015
Actual Primary Completion Date :
Oct 22, 2018
Anticipated Study Completion Date :
Dec 31, 2022

Outcome Measures

Primary Outcome Measures

  1. Assessment of Pharmacokinetic Glycopeptides Cmax [30 minutes after first injection]

    Evaluate the rate of patients for whom the objective of efficiency PK / PD Cmax / MIC ≥ 8-10 is reached at the first dose of the usual doses

  2. Assessment of Pharmacodynamic Glycopeptides Cmax [30 minutes after first injection]

    Evaluate the rate of patients for whom the objective of efficiency PK / PD Cmax / MIC ≥ 8-10 is reached at the first dose of the usual doses

  3. Assessment of Pharmacokinetic β-lactam-aminoglycoside Cmax [30 minutes after first injection]

    Evaluate the rate of patients for whom the objective of efficiency PK / PD Cmax / MIC ≥ 8-10 is reached at the first dose of the usual doses

  4. Assessment of Pharmacodynamic β-lactam-aminoglycoside Cmax [30 minutes after first injection]

    Evaluate the rate of patients for whom the objective of efficiency PK / PD Cmax / MIC ≥ 8-10 is reached at the first dose of the usual doses

Secondary Outcome Measures

  1. Mortality rate [Day 30]

    Compare the 30-day mortality among patients with subclinical a first rate versus those who have reached the desired peak

  2. Assess the residual of Glycopeptides [Hour 12 and Hour 24 after injection]

    Assess the residual to 12h after injection to an anticipation of residual dosed at 24.

  3. Assess the residual of β-lactam-aminoglycoside [Hour 12 and Hour 24 after injection]

    Assess the residual to 12h after injection to an anticipation of residual dosed at 24.

Eligibility Criteria

Criteria

Ages Eligible for Study:
18 Years and Older
Sexes Eligible for Study:
All
Accepts Healthy Volunteers:
No
Inclusion Criteria:
  • Age w< 18 years old

  • admitted in ICU unit for whom aminoglycoside treatment for severe infection was prescribed

Exclusion Criteria:
  • Age less than 18 years

  • Treatment with aminoglycoside off label

  • Patient non hospitalized in intensive care

Contacts and Locations

Locations

Site City State Country Postal Code
1 Groupe Hospitalier Paris Saint Joseph Paris Ile-de-France France 75014

Sponsors and Collaborators

  • Groupe Hospitalier Paris Saint Joseph

Investigators

  • Principal Investigator: Philippart Francois, MD, Groupe Hospitalier Paris Saint Joseph

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.
Responsible Party:
Groupe Hospitalier Paris Saint Joseph
ClinicalTrials.gov Identifier:
NCT02846298
Other Study ID Numbers:
  • PKPD AG-BL
First Posted:
Jul 27, 2016
Last Update Posted:
Mar 31, 2022
Last Verified:
Mar 1, 2022
Keywords provided by Groupe Hospitalier Paris Saint Joseph

Study Results

No Results Posted as of Mar 31, 2022