Abstract
Doripenem is a novel wide-spectrum antibiotic, and a derivate of carbapenems. It is an ideal antibiotic for treatment of serious nosocomial infections and severe sepsis for its exceptionally high efficiency and broad antibacterial spectrum of action. Doripenem is eliminated mainly by the kidneys. In cases of acute kidney injury, dosing of doripenem depends on creatinine clearance and requires adjustments. Doripenem is eliminated during hemodialysis because its molecular weight is 300–400 Da. The aim of this study was to establish the impact of continuous renal replacement therapy (CRRT) slow low-efficiency dialysis (SLED) on doripenem serum concentrations in a population of intensive-therapy patients with life-threatening infections and severe sepsis. Ten patients were enrolled in this observational study. Twelve blood samples were collected during the first administration of doripenem in a 1-hour continuous infusion while CRRT SLED was provided. Fluid chromatography was used for measurement of the concentration of doripenem in serum. In all collected samples, concentration of doripenem was above the minimum inhibition concentration of this antibiotic. Based on these results, we can draw the conclusion that doripenem concentration is above the minimum inhibition concentration throughout all of CRRT. The dosing pattern proposed by the manufacturer can be used in patients receiving CRRT SLED without necessary modifications.
Introduction
Doripenem, like other carbapenems, is an ideal antibiotic for treatment of serious nosocomial infections and severe sepsis for its exceptionally high efficiency and broad antibacterial spectrum of action. In microbiological studies, it showed high activity against some bacterial strains (eg, Pseudomonas aeruginosa, Klebsiella sp.) responsible for ventilator-associated pneumonia (VAP).Citation1 Clinical studies showed similar efficacies of doripenem and meropenem in the population of febrile patients with acute hematologic diseases.Citation2 A randomized controlled trial comparing a 7-day course of doripenem to a 10-day course of imipenem/cilastatin for VAP due to Gram-negative bacteria infection found no significant differences in efficacy or mortality rate.Citation3 Thus, doripenem is an important antimicrobial chemotherapeutic agent, especially for patients suffering from serious infections and severe sepsis caused by Gram-negative species. An analysis of patients with concurrent bacteremia and either nosocomial pneumonia, complicated intra-abdominal infection, or complicated urinary tract infection from six Phase III clinical trials demonstrated similar cure rates and clearance of bacteremia in patients treated with doripenem and comparator agents.Citation4 In the US CAPITAL (Carbapenem Antimicrobials Pseudomonas Isolate Testing At regional Locations) 2010 surveillance program, doripenem was found to be the most active carbapenem agent against P. aeruginosa (88.6% isolates susceptible versus 78.1% for imipenem and 84.6% for meropenem).Citation5
Doripenem is mainly eliminated by kidneys; thus, the dose adjustment in cases of renal failure is a necessary therapeutic modification. However, if patients are treated with the use of renal replacement therapy (RRT) technique, the drug elimination may increase significantly, and adequate dosage and administration is unclear.Citation6,Citation7 The growing role and increasing importance of RRT is based on the evidence that the early use of the procedure may limit mortality rate and improve outcome.Citation8 The molecular weight cutoffs of commonly used filter membranes are much higher than the molecular weight of unbound particles of antibiotics. Thus, the free fraction of antibiotics should be eliminated during RRT, with speed depending on modality and form of individually planned procedures. Additionally, the subsequent occurrence and growth of other elements of multi organ dysfunction syndrome (MODS) disturbances may significantly affect the pharmacokinetics of many drugs, among them doripenem and other antibiotics.Citation9 In such situations there is an important risk that increased RRT antibiotic clearance might create a competing morbidity, secondary to ineffective treatment of serious infections.Citation10 There are many continuous renal replacement therapy (CRRT) modes available, but for patients in severe sepsis slow low-efficiency dialysis (SLED) seems to be a good option. The main advantages of SLED technique for such patients are hemodynamic stability and effective reduction of the fluid overload.
The aim of this study was to establish the impact of SLED used as a CRRT on doripenem serum concentrations in a population of intensive-therapy patients with life-threatening infections and severe sepsis.
Materials and methods
After obtaining the ethics committee approval, the study began. The inclusion criteria were: severe sepsis, acute kidney injury (AKI) and failure (defined following RIFLE and AKIN criteria), and infection with bacteria sensitive to doripenem. The sensitivity was confirmed by antibiogram. Exclusion criteria were: lack of consent, possible allergy to carbapen-ems, and administration of carbapenem antibiotics prior to the study because they may interfere with chromatography measurement – the chemical structure of doripenem is similar to other carbapenems so it could affect the results of measurement of concentration of drug in serum. All included patients required RRT. The method used for this trial was SLED with Genius apparatus with high-flux filter. The dose of hemodialysis was individually determined, but generally all patients received one standardized session of RRT for trial: blood flow 120–130 mL/min and ultrafiltration 2,000–7,000 mL/24-hour (mean ultrafiltration 4,500 mL/24-hour). A standard dialysis fluid container capacity was 90 L, and during a 24-hour session the measured total fresh dialysate circulating volume was 180 L. For the study, a new session was always commenced with fresh dialysate fluid.
The study protocol was as follows: sample 0 was collected before administration of drug; the RRT session was started with a new container; doripenem was administrated in a 1-hour infusion using an automated syringe following recommendations of the manufacturer. Sample 1 was collected from separate intravenous access 30 minutes after commencing the drug administration during CRRT. Next, samples 2–8 were collected in 30-minute intervals for the first 4 hours, and samples 9–12 every 1 hour for the next 4 hours. Summary time of sample collection was 8 hours. Only the first administration of doripenem was evaluated.
Every sample was prepared following instruction for the fluid chromatography measurement: the blood samples were collected to vacutainer heparinized blood collection tube. Collected blood samples were centrifuged for 10 minutes (1,000× g) at a temperature of 4°C. Zero point five milliliters of serum was then taken into 2 mL Eppendorf testing tubes and mixed with 0.5 mL of 1 mol/L 3-(N-morpholino)propanesulfonic acid buffer. Then, it was stored in a −40°C refrigerator until the time of analysis. The analysis was performed on a fluid chromatography machine. Blood samples were subjected to spectrophotometric detection using ultrafast performance liquid chromatography using the ACQUITY ultrafast performance liquid chromatography (BEH C-18, 100x2,1 mm; Waters Inc., MA, USA) column to determine the concentrations of doripenem.
Statistical analysis was performed using Microsoft Office Excel Package (Microsoft Corporation, Redmond, WA, USA).
Results
Department of Anesthesiology and Intensive Therapy at Barlicki University Hospital is referral for the regions intensive care unit (ICU) which has 13 beds. The severe sepsis cases are admitted from the area of Lodz city and its surroundings. There are five Genius machines for CRRT. The mean number of patients admitted to this ICU was 304 per year, mean time of treatment was 9.8 days, and mean mortality rate was 64.1%.
The study was commenced in 2008. In 2008, a total of 309 patients were admitted to this ICU; in 2009, 303 patients were admitted; and in 2010, 306 patients were admitted. The number of performed SLED/CVVHD procedures was 168 (in 2008), 222 (in 2009), and 231 (in 2010) in a total of 78 patients. Forty-nine of them suffered from severe sepsis, but 39 required CRRT. Inclusion criteria (severe sepsis, MODS, AKI, and infection caused by bacteria sensitive to doripenem) as well as no carbapenem administration prior to the study was met by 16 patients. Finally, it was possible to include 14 adult patients (seven men and seven women) into the study. Complete data were collected for ten of the patients who met the inclusion criteria (six men and four women). Demographic data, scoring, and initial biochemical parameters (at the moment of commencing CRRT) are presented in . From ten patients, included into the study, nine died and one survived. In , reason for admission (main illness causing sepsis) and comorbidities are presented. All patients included suffered because of severe sepsis or septic shock secondary to diagnosed infections (mean serum c-reactive protein 236.9±92.8 mg/L, mean serum procalcitonin 102±116.6 ng/mL, white blood cell count 39.4±19.0 g/L, platelet blood count 66.1±56.8 g/L) and had need for advanced mechanical ventilation with the use of high fraction of inspired oxygen (0.85±0.25) and catecholamine infusions. Additionally they all suffered because of significant acute nutrition disorders (with mean serum protein 41.75±14.37 g/L), which were resistant to applied alimentation therapy (supplemented both via parenteral 1,690±637 mL/day and enteral 1,004±603 mL/day route, with maximum achieved serum protein 44.51±14.19 g/L). Most of them had need for blood products transfusions (18.5±26.6 units) secondary to surgical procedures, gastrointestinal bleedings, and disseminated intravascular coagulation. Administered targeted antibiotic therapy with the use of doripenem led in three cases to selection of carbapenem-resistant species of Acinetobacter baumannii, which were treated with the use of intravenous and nebulized colistin (according to laboratory-tested susceptibility). The main causes of the high mortality rate were relatively late admission into the clinical ICU (all patients included were previously treated without effects in other wards, ICUs, and hospitals) and irreversible damage of at least one of the main vital organs (central nervous system, heart, or lungs) that was resistant to applied therapy.
Table 1 Demographic data, ARF parameters at date of study, and length of stay at ICU
Table 2 Main illness causing sepsis and comorbidities
The mean concentrations of doripenem in serum are presented in . In all collected samples, concentration of doripenem was above minimum inhibition concentration of antibiotic (MIC) for doripenem.
Figure 1 Mean concentration of doripenem in serum.
Discussion
It is estimated that up to 40% of ICU patients may develop AKI and 5% of them will require RRT. The majority of them have infection and multiorgan dysfunction. Sepsis accompanied with AKI is an indication for CRRT.Citation11 AKI criteria are met when blood urea nitrogen exceeds 80 mg/dL or creatinine level is above 3 mg/dL.Citation11 All patients included in our study met the criteria of AKI and severe sepsis. They all suffered due to: respiratory failure (required mechanical ventilation), circulatory failure (required vasopressors and fluid therapy), and other systems disturbances (metabolic disorders, drop in platelet count and elevation of c-reactive protein and lactate levels). Most importantly, they had severe infection. This severe infection required adequate treatment including antibiotic therapy. AKI was treated with the use of RRT. The best option for ICU patients, especially those suffering from cardiovascular instability, is CRRT because it has less effect on the cardiovascular system than standard hemodialysis provided as intermittent hemodialysis (IHD) and creates a much more effective method for water elimination, which is essential for avoiding massive fluid overload aggravating mortality rate. In cases of standard hemodialysis, the modification of drug dosage for many antibiotics is well described, but as for CRRT there are not many pharmacology studies and those available were performed on small groups of patients – for example, for carbapenems (imipenem), six patients were included for one method of CRRT.Citation12 Available recommendations for antibiotics dosage during CRRT are based on very limited clinical data, and in many cases, those dosing recommendations are extrapolations from clinical experiences and known pharmacokinetic and pharmacodynamic properties. More clinical data are needed to support such extrapolations, and these recommendations should not supersede sound clinical judgment.Citation13 So it is still not well-known how to modify doses of some antibiotics in patients with MODS, AKI, and sepsis undergoing CRRT. Because there are several methods of CRRT available it complicates the situation even more. It is indicated to measure levels of antibiotics in serum during therapy, as the best method of adjusting dosage, but this is not available in many hospitals because of the high level of costs and complicated procedures. The way of dosing antibiotics differs between IHD and CRRT.Citation14 As mentioned before, methods of CRRT are also different; for example, continuous venovenous hemofiltration (CVVH) will influence in different ways antibiotic concentration in serum compared to the SLED technique. Type of filter also plays an important role in elimination of antibiotics. In the case of all mentioned methods of RRT, extracorporeal elimination of drugs is different. In cases of patients treated in ICU, the situation is more complicated because of changes in pharmacology of drugs; for example, changes in albumin levels and their composition influences protein binding of drugs which is important for elimination fraction during RRT.Citation14 Those changes in pharmacokinetics of drugs are connected with pathophysiology in the course of illness (for example, disseminated intravascular coagulation, endothelium leakage, changes in serum proteins, and acid–base balance disturbances) and interactions with drugs used for therapy. As a consequence, it is observed that changes in volume of distribution of water-soluble drugs, altered protein binding, levels of free fraction of drugs, and altered metabolism of drugs and other substances (including for example hormones, decreased clearance, and hyperdynamic circulation in early sepsis) may result in supranormal renal clearances.Citation15 All of this makes antibiotic therapy difficult in severely ill patients. Antibiotic therapy requires usage of algorithms of drug dosage and special formulas for modification. The general rule is that during CRRT, as it is less efficient than IHD, the drug dosage may not be changed.Citation16 But still it was not proved in the case of CRRT SLED that this approach is correct.Citation15 The molecular weight of the majority of antibiotics is lower than 1,500 Da (many of them have a molecular weight lower than 500 Da) and they are easily removed during extracorporeal elimination. Protein binding is very important because only the free fraction of antibiotics is removed during CRRT SLED. If protein binding is less than 80%, the antibiotic is also easily eliminated. Clearance of most of antibiotics is high during CRRT, but in cases of CRRT SLED, because it is low-efficiency dialysis, the dosage may not be required to be modified. If extracorporeal elimination of drug is higher than 25%, the modification in dosage may be necessary. If drug concentration in serum is lower than minimal bactericidal concentration (MBC), there is a serious risk of developing drug resistance of bacteria, so the aim of antibiotic dosing pattern must be keeping levels of antibiotic concentration in serum above MBC. Thus, for antibiotics with low toxicity, the overdosage during CRRT may be required to keep serum concentration above MBC. This is not proved for CRRT SLED. In a previously published study on antibiotic therapy during SLED among chronic stable patients, underdosing was common.Citation17 But up to this moment there are no published studies on doripenem dosage in cases of critically ill patients undergoing CRRT SLED.
Doripenem is a novel wide-spectrum antibiotic and a derivate of carbapenems. It was introduced to clinical practice in 2005 in Japan, and in 2008 in Poland. In carbapenems, classification of doripenem is situated in group 2 together with meropenem and imipenem.Citation18 Doripenem is especially useful in treatment of infections that are methicillin or vancomycin resistant. It is used in complicated intra-abdominal infections, complicated urinary-tract infections, severe community associated pneumonia, severe hospital-associated pneumonia, and VAP/intubated-associated pneumonia.Citation19 Therefore, it is much needed in ICUs and has very good activity on isolates of P. aeruginosa (importantly, it has lower MIC90 than meropenem and imipenem). It provides less selection of carbapenem-resistant P. aeruginosa metallo-beta-lactamase and has lower toxic effect on the central nervous system.Citation20,Citation21 The pharmacological properties of doripenem are: half-life of 1 hour, low protein binding (8.1%), high concentration of active form in serum, and it is stable toward dehydrogenase I. Thirty percent of the drug is metabolized and 70% is removed unchanged through kidneys within 24 hours.Citation18 Like other carbapenems, doripenem has time-dependent pharmacokinetics/pharmacodynamics – %T>MIC. The effectiveness is high with serum maximum concentration 4–5 times bigger than MIC and concentration above the MIC maintained through more than 40% of time between dosages. Doripenem may be administrated in a 1-hour infusion (three times 500 mg) or in prolonged 4-hour infusion (extended infusion dosing) which increases significantly %T>MIC.Citation18 Maximum concentration of drug when dosed as mentioned reaches 23 μg/mL. MIC for Enterobacteriaceae is 4 μg/mL, and for resistant P. aeruginosa 16 μg/mL.Citation22 In renal failure, dosing of doripenem depends on creatinine clearance and requires adjustments.Citation23 Doripenem is eliminated during hemodialysis because its molecular weight is 300–400 Da.Citation23 Standard filters used for CRRT SLED have pores of 1,200 Da size.
The studies on doripenem pharmacokinetics in patients undergoing CRRT showed that, depending on the procedure technique (CVVH versus CVVHD), administered dose removal varied from 38% to 29%. Thus, doripenem dosage regimens for patients receiving CRRT need to be adjusted.Citation23 Only a few studies involving critically ill patients treated with doripenem and receiving CRRT have been published up to this moment. Different populations and techniques of CRRT described in these studies may have an important impact on the results. Additionally the involved study populations were very small. Ohchi et al concluded that clearance via hemodiafiltration increases proportionally to the hemopurification rate. Thus, they suggested that doripenem dose should be increased to 1.0–1.5 g/day in critically ill adults when performing high-flow continuous hemodiafiltration.Citation24 From the same center, Hidaka et al reported previous to this that the blood level of doripenem can be satisfactorily controlled by adjustment of doripenem dose and dosing interval, in accordance with residual renal function in critically ill patients receiving standard continuous hemodiafiltration.Citation25 On the other hand, Samtani et al suggested that a reduction in doripenem dose will be needed for critically ill patients receiving CVVH or continuous venovenous hemodiafiltration.Citation26 Up to this moment, there are no studies published on the patients treated with doripenem and receiving CRRT in SLED mode. The results from our study may improve safety and efficacy of doripenem therapies in the population of critically ill patients.
Conclusion
Based on these results, we can draw the conclusion that concentration of doripenem is above MIC for this antibiotic throughout CRRT. The dosing pattern proposed by the manufacturer can be used in patients receiving CRRT SLED without necessary modifications.
Acknowledgments
We would like to thank Dr Slawomir Brzeznicki from the Department of Toxicology Medical University of Lodz, Poland, for preparing methods and performing fluid chromatography measurements. The trial was conducted with government grant number: N N403 185434. 507-16-027.
Disclosure
The authors report no conflicts of interest in this work.
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