Gram-Negative Bacterial Infections Clinical Trial
Official title:
An Observational Pharmacokinetic Sudy of Ceftolozane-Tazobactam in Intensive Care Unit in Patients With and Without Continuous Renal Replacement Therapy.
The purpose of this study is to try to find out how critically ill patients receiving the
antibiotic, ceftolozane-tazobactam, process it in their body. Investigators would like to
study if the antibiotic concentrations during a dose of this antibiotic reaches the right
concentrations necessary to kill the bacteria that is causing the infection. The process by
which a drug travels through the body in blood, how it is broken down and removed by the body
is called pharmacokinetics (PK). We can measure the PK by taking blood samples at specific
times after the antibiotic is given.
Investigators would like to do the study in patients receiving dialysis and patients who are
not receiving dialysis. This information about how the antibiotic is processed in the
critically ill patient is unknown and it is important to know whether the doses doctors give
patients to fight infection are adequate. If antibiotic concentrations are low in the blood,
it gives the bacteria an opportunity to become resistant to the antibiotic which can lead to
the antibiotic being less effective against bacteria potentially exposing future patients
with infections to a limited range of effective antibiotics.
Patients will be consented, and given the antibiotic as prescribed. Blood samples will be
taken from the drip that is already in the patients arm just as the antibiotic starts, at 15
and 45 minutes, at 1,2,3,4,5,6,7 and 8 hours. Patients who are on dialysis will have the
blood samples taken from the dialysis machine before the blood reaches the dialysis filter
(same blood samples as the non dialysis patients) and also bloods samples taken after the
filter at 45 minutes, 2 and 6 hours. Dialysis patients will also have 5 separate samples of
ultrafiltrate taken (approximately 10mls) - ultrafiltrate is the waste product of the
dialysis process. The total amount of blood will be 40mls which is equal to about 2
tablespoons. The dialysis patient will have 50mls of blood taken.Information about the
patients ICU stay will also be recorded.
Ceftolozane-tazobactam has recently emerged as a highly valuable option for the management of
severe Gram-negative infections including those caused by multi-drug resistant (MDR)
organisms, demonstrating superior antibacterial activity against the pathogens most
frequently causing serious infection in the critically ill, such as Pseudomonas aeruginosa
and Enterobacteriaceae spp, when compared with other commonly used beta-lactam antibiotics.
Although the continued reduction in the pathogen susceptibility to commonly used antibiotics
in ICUs could be multifactorial, the potential contribution from inappropriate antibiotic
exposure is undoubtedly very significant. Numerous clinical studies have reported
sub-therapeutic antibiotic concentrations in ICU patients across different antibiotic
classes, with conventional dosing regimens. This is due to marked changes in the
pharmacokinetics (PK) and pharmacodynamics (PD) of antibiotics in the critically ill arising
from disease-related physiological changes. Ceftolozane being a structural analogue of
ceftazidime, shares similar PK properties of ceftazidime, and other beta-lactams, with a
short half-life of about 2 hours, distribution into extracellular fluid, and predominant
renal elimination, which all make it vulnerable to disease-related PK alterations in the
critically ill.
Inappropriate antibiotic exposure in the ICU can also arise due to use of extracorporeal
therapies such as continuous renal replacement therapy (CRRT). Many beta-lactam antibiotics
share similar physicochemical and PK properties with ceftolozane and are efficiently cleared
by CRRT machines. However the extent of total drug clearance during CRRT is variable not only
due to the different modalities and operational settings across different institutions, but
also due to the variable residual renal clearance associated with the degree of renal
impairment. The traditional dosing considerations in patients undergoing CRRT mainly focus on
the notion of renal impairment and generally consider low doses without giving appropriate
consideration to the possibly high extracorporeal clearance, and thus risking under dosing.
In a similar fashion, the product information for ceftolozane-tazobactam or the prescriber's
information by the United States Food and Drug Administration (FDA), recommends a ten-fold
lower-than-normal dose for use during renal replacement therapy (maintenance dose of 150mg
versus 1.5g in those with normal renal function). However, to date there is limited data from
clinical studies during CRRT in ICU patients to confirm if such a low dose provides
appropriate antibiotic exposure. Lessons from studies on other beta-lactams suggest that
ceftolozane may be subject to extensive but variable clearance during CRRT. It is therefore,
essential to describe the adequacy of dosing in patients receiving CRRT, given that fact and
that several additional pathophysiological factors affect the PK and PD of antibiotics even
in the absence of extracorporeal circuits.
This prospective observational study will describe, firstly, the PK of ceftolozane-tazobactam
in ICU patients who are not receiving CRRT, and secondly, the influence of CRRT on the PK and
dosing requirements of ceftolozane-tazobactam in critically ill patients. This study will
generate new PK data in ICU patients describing the exposure to ceftolozane-tazobactam from
the recommended dosing regimen thereby allowing assessment of its adequacy and/or defining
appropriate dosing. Further, it will provide invaluable insight into the altered dosing needs
of patients receiving CRRT to enable its use in such patients through prediction of any
necessary dosing corrections to account for the due effect of CRRT.
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