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NCT03133910 Clinical Trial

Pharmacokinetics and Pharmacodynamics of Ceftazidime in Pediatric ICU Patients

Sepsis Clinical Trial

Official title:
Pharmacokinetics and Pharmacodynamics of Ceftazidime in Pediatric ICU Patients

Clinical Trial Details — Status: Enrolling by invitation

Administrative data
NCT number NCT03133910
Other study ID # 2016-679
Secondary ID
Status Enrolling by invitation
Phase N/A
First received March 9, 2017
Last updated April 25, 2017
Start date March 9, 2017
Est. completion date January 2019

Study information
Verified date April 2017
Source Ann & Robert H Lurie Children's Hospital of Chicago
Contact n/a
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Mortality benefit has been proven with early antibiotic administration in sepsis. Antimicrobial therapy should be based on early achievement of effective drug concentrations by optimizing the pharmacokinetic/pharmacodynamics of individual drugs. Optimal dosing in the critically ill patient can be challenging with the rapidly changing physiology of sepsis during the first days of hospitalization with capillary leak, fluid overload, changes in cardiac output, and alterations renal clearance. Ceftazidime is the preferred beta-lactam for empiric treatment of sepsis at Lurie Children's Hospital because of its anti-pseudomonal and anti-enteric bacilli coverage, however, the majority of pharmacokinetic data currently published in pediatrics does not include Intensive Care Unit (ICU) patients. Adult pharmacokinetic/pharmacodynamics data suggest that critically ill adults with high level of illness severity may benefit from continuous or extended infusion beta lactam therapy to optimize the therapeutic concentration particularly for pathogens that are relatively resistant to beta-lactams. Understanding the changing pharmacokinetic/pharmacodynamics of ceftazidime with the progression of illness in the ICU may help determine if current dosing regimens are adequate to maintain appropriate drug concentrations to optimize antimicrobial treatment.

Description:

Severe sepsis continues to be a leading cause of admission and death in the pediatric critical care population. Mortality benefit has been proven with early antibiotic administration. Optimal antimicrobial therapy should be based on early achievement of effective drug concentrations by optimizing the pharmacokinetic/pharmacodynamics of individual drugs. Ceftazidime is the preferred beta-lactam for empiric treatment of sepsis at Lurie Children's Hospital because of its anti-pseudomonal and anti-enteric bacilli coverage, however, the majority of pharmacokinetic data currently published in pediatrics does not include ICU patients. For beta-lactams like ceftazidime, the time that free (nonprotein bound) drug concentration remains above the minimum inhibitory concentration (MIC) of the bacteria (t>MIC) best defines the bacteriostatic and bactericidal activity. Based on previous animal studies and subsequent clinical studies, beta-lactams require about 50% t>MIC. Adult pharmacokinetic/pharmacodynamics data suggest that critically ill adults with high level of illness severity may benefit from continuous or extended infusion beta lactam therapy to optimize time above MIC particularly for pathogens that are relatively resistant to beta-lactams. Positive outcome results using extended infusion have been found with respect to mortality benefit, clinical cure, reduced length of stay, and increased ventilator free days. It is likely that because children experience changes in physiology with critical illness likely leading to alteration in antibiotic clearance, additional data are needed to determine if our current dosing strategies are achieving optimal antimicrobial exposure. Understanding the changing pharmacokinetic/pharmacodynamics of ceftazidime with the progression of illness in the ICU may help determine if current dosing regimens are adequate to maintain appropriate t>MIC. In this study all patients between the ages of 2 months and 18 years admitted to the Pediatric Intensive Care Unit/ Cardiac Intensive Care Unit (PICU/CICU) who will receive ceftazidime for empiric or definitive antimicrobial therapy with an expected duration of greater than or equal to 48 hours who meet inclusion criteria will be enrolled in this prospective, non-interventional, pharmacokinetic study. Sampling of serum to determine concentrations will occur around ceftazidime doses during the first 48 hours after admission or onset of hospital associated illness, with additional sampling up to 7 days if antibiotic use continues. Using a traditional FDA-approved dosing regimen (50 mg q 8hr with maximum dosing of 6g/d), samples will be drawn following the 2nd or 3rd dose of Ceftazidime received by the patient at times: 0 min (predose), 30 min, 1 hour, and 4 hours following dose. During the second 24 hours of therapy, one sample will be drawn between hours 2 and 4 post dose and if therapy continues additional samples will be drawn daily between hours 2 and 4 post dose up to 7 days. Additional information will be collected to better assess volumes of distribution, drug clearance, kidney function, and cardiac output to determine patient covariates that may help delineate which patient populations associated with altered ceftazidime exposure. Population pharmacokinetic modeling will be performed and various regimens will be simulated to identify optimal dosing.

Recruitment information / eligibility
Status Enrolling by invitation
Enrollment 20
Est. completion date January 2019
Est. primary completion date January 2018
Accepts healthy volunteers No
Gender All
Age group 2 Months to 18 Years
Eligibility Inclusion Criteria:

- Admitted to pediatric or cardiac intensive care unit

- Between the ages of 2 month to 18 years

- Receiving ceftazidime for an anticipated course of greater than or equal to 48 hours

- Central venous or arterial access for blood sampling

Exclusion Criteria:

- Less than 2 months or greater than 18 years

- Anticipated need for renal replacement therapy or ECMO

- History of chronic kidney disease greater than stage 1

- Inadequate access for blood draws

Study Design

Related Conditions & MeSH terms

Locations
Country Name City State
United States Ann & Robert H Lurie Childjren's Hospital of Chicago Chicago Illinois

Sponsors (2)
Lead Sponsor Collaborator
Ann & Robert H Lurie Children's Hospital of Chicago Northwestern Memorial Hospital

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Primary Duration of time that antibiotic concentration is above the minimum inhibitory concentration (T>MIC) of common gram negative bacteria Number of patients with altered ceftazidime concentrations due to critical illness as measured by less that 50% T>MIC. Blood sample collection beings within 24 to 32 hours of antibiotics administration. Day 1 collections times are zero (predose); 30 minute post dose; 1 hour post dose; 4 hour post dose. Day 2 through 7 collections times occur 2 to 4 hour post dose.
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