The study aims to compare the efficacy, safety and pharmacokinetics (PK) of an optimised dosing to a standard dosing regimen of vancomycin in neonates and infants aged ≤ 90 days with late onset bacterial sepsis known or suspected to be caused by Gram-positive microorganisms
Detailed objectives of the study are: * To compare the efficacy of an optimised vancomycin dosing regimen to a standard vancomycin dosing regimen in patients with late onset, bacterial sepsis, known or suspected to be caused by Gram-positive microorganisms. * To compare the safety of vancomycin (including renal and hearing safety) by allocation group in the intention to treat (ITT) population * To describe the PK parameters according to vancomycin dosing regimen and outcome using population PK modelling in the ITT population * To describe PK/PD in terms of the probability of target attainment (PTA) with different vancomycin dosing regimens in the ITT and per protocol (PP) populations * To describe outcomes and duration of therapy at the end of vancomycin treatment and at the short term follow-up visit by allocation group in the ITT and PP populations * To compare the clinical outcome to the antibacterial susceptibility of infecting organisms * To compare colonisation by resistant microorganisms (e.g. vancomycin-resistant enterococci (VRE)) and Candida spp. by allocation group at baseline, TOC and short-term follow-up * To validate across multiple centres a host biomarker panel to allow improved diagnosis of bacterial sepsis and monitor response to antibacterial therapy
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
NONE
Enrollment
242
Vancomycin is an antibiotic used to treat a number of bacterial infections.It is recommended intravenously as a treatment for complicated skin infections, bloodstream infections, endocarditis, bone and joint infections, and meningitis caused by methicillin-resistant S. aureus.
Tallinn's Children's Hospital
Tallinn, Estonia
Paediatric Intensive Care Unit, Clinicum of the University of Tartu
Tartu, Estonia
Successful outcome at Test of Cure visit
Patient is alive AND has a successful outcome at the end of actual vancomycin therapy AND the patient has not had a clinically or microbiologically significant relapse or new infection.
Time frame: 10±1 days after End of Actual Vancomycin Therapy
Clinically or microbiologically significant relapse or new infection requiring treatment with any other antibiotic for more than 24 hours
Time frame: 10±1 days after the End of Actual Vancomycin Treatment
Successful outcome at Visit 4 or End of Actual Vancomycin Therapy including total duration of vancomycin therapy
Time frame: Day 5±1 or Day 10±2
Abnormal renal function tests at the Short-term Follow-Up Visit
Time frame: 30±5 days post-initiation of vancomycin therapy
Abnormal hearing screening test
Time frame: By Day 90 post-initiation of vancomycin therapy
Comparative safety of vancomycin (relating to the number of treatment-related adverse events other than those associated with renal function and hearing) at Short Term Follow-Up Visit
Time frame: 30±5 days post-initiation of vancomycin therapy
Pharmacokinetic parameters of vancomycin using population PK modelling by allocation group
Area under the plasma concentration time curve - AUC (mg\*hour/L)
Time frame: Up to 2 years (final data collection date for outcome measure)
Probability of target attainment (PTA) with different study regimens
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Aghia Sophia Children's Hospital (A)
Athens, Greece
Aghia Sophia Children's Hospital (B)
Athens, Greece
Aghia Sophia Children's Hospital (C)
Athens, Greece
Kyriakou Children's Hospital
Athens, Greece
General University Hospital Attikon
Chaïdári, Greece
Hippokration Hospital - Department of Neonatology
Thessaloniki, Greece
Papageorgiou 2nd Department of Neonatology
Thessaloniki, Greece
Ospedale "Di Venere" - Carbonara di Bari
Bari, Italy
...and 8 more locations
Different bacteriological targets will be tested, based on the MIC of different bacteria of interest with level of sensitivity. Simulations based on the vancomycin popPK model will be conducted to define the number of patients in the different allocation groups reaching the predefined targets when modifying the dose.
Time frame: Up to 2 years (final data collection date for outcome measure)
Relationship between CoNS species and duration of treatment and CRP response
Time frame: Day 5±1 or Day 10±1
Gut colonisation by vancomycin resistant organisms at baseline, Test of Cure Visit and Short-term Follow-Up Visit
Time frame: Baseline, 10±1 days after end of vancomycin therapy, 30±5 days post-initiation of vancomycin therapy
Skin colonisation and resistance patterns before and after vancomycin treatment
Time frame: Baseline, 10±1 days after end of vancomycin therapy, 30±5 days post-initiation of vancomycin therapy
Assessment of changes in host biomarker panel profiles from baseline to End of Actual Vancomycin Therapy and the relationship between host biomarker and duration of treatment
Functional molecular units based on a multimarker panel - a set of 52 biomarkers will be performed as a classifier with high accuracy and specificity in predicting bacterial infection
Time frame: Day 3 and Day 5±1, Day 10±1 (standard arm only)