Pneumonia, Ventilator-Associated Clinical Trial
Official title:
Randomised, Open-Label Clinical Trial on The Efficacy of Colistin Plus Rifampicin Treatment Versus Colistin Alone for Severe Infections Due to Multidrug-Resistant Acinetobacter Baumannii
Acinetobacter baumannii causes severe infections (pneumonia, bacteremia, organ space) with
high lethality in hospitalised critically ill patients. It can acquire resistance to all
classes of antibiotics (multidrug resistance, MDR) except an 'old' drug, colistin, which may
be the only therapeutic option. However, colistin is not registered for this indication. The
addition of rifampicin to colistin has been shown to be synergistic in vitro, and may be
promising in vivo, but this combination has not been studied in comparison with colistin
alone.
The purpose of this randomised, open-label, multicentre clinical trial is to assess whether
the association of colistin and rifampicin reduces significantly the mortality of patients
with severe MDR A. baumannii infections compared with colistin alone.
The trial will enroll 210 patients from intensive care units (ICU) of five tertiary care
hospitals where MDR A. baumannii infection is endemic with epidemic phases. Patients will be
randomly allocated to either colistin alone (control arm) or colistin plus rifampicin
(experimental arm).
Primary end point is overall mortality, defined as death occurring within 30 days from
randomisation.
Secondary end points will be disease-specific death, microbiological eradication,
hospitalization length, emergence of resistance to colistin during treatment.
This study is designed as a multicentre open-label, parallel randomised, controlled trial.
Patients will be randomly allocated to two treatment arms: 1) colistin alone (control arm);
2) colistin, plus rifampicin (experimental arm). The study will be carried out over 2 years
according to the principles of good clinical practice.
The study population is represented by adult hospitalised patients with severe nosocomial
infections due to multi-drug resistant A. baumannii, susceptible to colistin. It will be
performed in intensive or sub-intensive care units of 5 Italian clinical centres where MDR
A. baumannii infection is endemic with epidemic phases. All adult subjects, irrespective of
age, will be included in the study, thus also elderly subjects will be eligible. Large
eligibility criteria are warranted by the pragmatic approach of the study, the severe
prognosis of these patients and the lack of effective alternative treatments.
Enrollment procedure: At the time of A. baumannii isolation, inclusion and exclusion
criteria will be checked by the pertinent centre.
Once obtained the informed consent, subjects will be randomized to treatment. No patient may
be enrolled in a centre before the formal approval of the Ethics Committee of that
Institution.
Accrual time: according to the sample size estimate (see below) and based on the current
incidence of MDR A. baumannii severe infections of 12-14 cases per month in the five
participating centres, the accrual time will last approximately 18 months to achieve the
planned sample size.
Severe infections include hospital acquired pneumonia (HAP), ventilator associated pneumonia
(VAP), bloodstream infection, intra-abdominal infection or other organ-space infections.
Multi-drug resistant A. baumannii is defined as clinical isolates resistant to carbapenems
and to all other antimicrobial drug classes, except colistin, irrespective of rifampicin
activity.
Severity of illness is assessed by the SAPS II score. This will be considered low or high
according to a SAPS II score below/equal to or higher than 40, respectively.
Patients will be randomly allocated into two treatment arms: 1) colistin alone, 2 million
units every 8 hours intravenously or according to renal function (control arm); 2) colistin,
2 million units every 8 hours intravenously or according to renal function, plus rifampicin,
600 mg every 12 hours intravenously (experimental arm).
Treatment will be administered for at least 10 days and up to a maximum of 21 days. Duration
of treatment will be established by the physician in charge. The end of treatment (EoT)
evaluation will be performed the day of treatment discontinuation. The end of study (EoS)
(follow-up) evaluation will be performed 30 days after randomization.
Treatment will be discontinued in the following instances: clinical cure with or without
microbiological eradication; occurrence of significant renal or liver toxicity; patient
death. Throughout the study, patients will receive routine intensive care support by the
physician in charge according to standard diagnostic and therapeutic guidelines.
Clinical cure is defined by disappearance of symptoms and signs of infection, irrespective
of A. baumannii eradication at the site of infection. Therapeutic failure is defined as
worsening or no improvement of clinical conditions on therapy with persistently positive A.
baumannii cultures.
Renal and liver function will be monitored by daily measurements of creatinine,
aminotransferase and direct bilirubin serum levels.
Drug dosages will be adjusted according to renal and liver function. Renal toxicity is
defined as decrease of creatinine clearance below 50 ml/min or >50% reduction in the
creatinine clearance relative to the baseline. Hepatic toxicity is defined as increase of
direct bilirubin above 3 mg/dl.
Surveillance cultures from the original source of isolation (blood, bronchial aspirate,
urines or drainage fluids) will be obtained on admission and repeated weekly, or whenever
clinically needed, during and after treatment to monitor persistence versus eradication of
A. baumannii at the infected site. In vitro activity of colistin and rifampicin will be
checked against all A. baumannii repeat isolates to detect development of resistance.
Identification and antibiotic susceptibility of A. baumannii isolates will be performed at
each centre using an automated system. Species identification will be confirmed by molecular
biology.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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