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. 2009 Jul 13;13(4):165. doi: 10.1186/cc7935

When once is not enough – further evidence of procalcitonin-guided antibiotic stewardship

Stephan Harbarth 1,, Werner C Albrich 2, Beat Müller 2
PMCID: PMC2750139  PMID: 19664168

Abstract

Every day, critical care physicians around the world face the same challenge of the optimal timing of antimicrobial administration: when to start and when to stop antibiotics. Duration of antibiotic therapy for sepsis is mostly based on expert opinion, but its reduction is arguably the most promising approach to decrease emergence and selection of antibiotic resistance. The study by Hochreiter and colleagues presents another piece of evidence suggesting that procalcitonin may indeed be a valuable diagnostic parameter to guide antibiotic treatment duration, despite the ongoing controversy about the diagnostic accuracy of pro-calcitonin.

In the previous issue of Critical Care, Hochreiter and colleagues presented another piece of evidence suggesting that procalcitonin (PCT) may indeed be a valuable diagnostic parameter to guide antibiotic treatment duration [1].

Misuse of antimicrobial agents has been a long-lasting problem in intensive care units (ICUs). Drivers of inappropriate prescribing include diagnostic uncertainty, lack of knowledge, unavailability of microbiologic support or infectious disease specialists, pharmaceutical marketing pressure, and the overarching fear of missing a life-threatening infection. Every day, critical care physicians around the world face the same challenge of the optimal timing of antimicrobial administration: when to start and when to stop antibiotics.

The duration of antibiotic therapy for sepsis is mostly based on expert opinion [2], but its reduction is arguably the most promising approach to decrease emergence and selection of antibiotic resistance. During the past 10 years, great progress has been made to decrease the antibiotic treatment duration for various types of infections, including community-acquired pneumonia and ventilator-associated pneumonia, by implementing fixed 8-day stopping rules [3,4]. A more tailored approach could be the use of algorithms based on the longitudinal course of biomarkers to facilitate individual decision-making and choose the right moment for discontinuation of antibiotic therapy.

At the current moment, PCT represents the best studied biomarker for guiding antibiotic treatment duration in the inhospital setting. Several randomized clinical trials investigating the diagnostic performance and clinical effectiveness of PCT have been published within the past 5 years or are currently submitted for publication [5-11]; however, few of them included a sufficient number of patients with severe sepsis and septic shock. In several of these studies, ICU admission was considered an acceptable criterion to overrule the PCT-based algorithm and initiate antibiotic therapy despite low PCT levels. Nobre and colleagues have shown recently that the application of an algorithm based on PCT levels allowed significant shortening of the duration of antibiotic therapy and of the ICU stay in critically ill patients with life-threatening infections, without apparent harm to patients [10].

In their article, Hochreiter and colleagues published the English translation of another randomized clinical trial of critically ill patients with different types of infections [1], confirming the study findings by Nobre and colleagues [10]. The original version of the Critical Care article has already been published in German in a peer-reviewed journal [12] and the analysis of a slightly different subgroup of patients has also been reported previously [13]. The major finding of these three articles is almost identical and relates to the reduction of the average antibiotic treatment duration and length of ICU stay by about 2 days.

The study by Hochreiter and colleagues was larger than previously published PCT trials conducted in the ICU setting. Some issues, however, warrant further comment. First, although it is likely that the reduction effect was mainly caused by the study intervention (PCT algorithm), it remains unclear in how many cases the PCT algorithm was forced into action by the study physicians or was overruled by the physicians in charge.

Second, the precise microbiologic etiology of the causative organisms and the documented relapse rate, secondary infections or other complications such as reoperations were not mentioned. It is conceivable that several cases of pneumonia or peritonitis were bacteremic or had a more complicated course, leading to potential antibiotic underuse and/or reintroduction at a latter time point. Given the heterogeneity of the included patients and infectious syndromes, a uniform 8-day antibiotic course for the control group might not reflect the standard of care for all indications. Indeed, it was different from the treatment approach for the control group in the previously reported subgroup analysis by the same authors, where 'treatment was discontinued according to clinical signs and empiric rules' [13].

Third, the study methods do not explain how the clinicians were blinded to the PCT values in the control arm, in order to avoid a spillover effect. How investigators were blinded for outcome assessment to avoid differential misclassification bias is also not described.

Fourth, the investigators used an insensitive PCT assay, which has been replaced in many settings by a more sensitive assay, considered more suitable for guiding antibiotic treatment decisions and for determining treatment-stopping rules [14].

Finally, it would have been interesting to know whether PCT is now implemented in their ICU as a routine parameter for the daily follow-up and how this practice influences real-life treatment decisions, outside a controlled study setting. There is potential for PCT overuse, as with all diagnostic tools, increasing expenditures due to the still-high costs of this test and unforeseen adverse consequences if used indiscriminately.

Despite these limitations, the study by Hochreiter and colleagues presents another piece of evidence suggesting that PCT may indeed be a valuable diagnostic parameter to guide antibiotic treatment duration. Seven randomized clinical trials about the diagnostic effectiveness of PCT have currently been completed [5-11], and several more are being conducted in different parts of the world, according to international trial registers http://clinicaltrials.gov/ct2/results?term=procalcitonin. Preliminary data from some of these trials are available and confirm the safety and efficacy of PCT guidance.

In summary, all these data from randomized clinical trials are good news for ICU physicians, despite the ongoing controversy about the diagnostic accuracy of PCT [15,16]. Clearly, we need even better diagnostic decision support tools if we want to help clinicians in their daily struggle for improving antibiotic treatment decisions.

Abbreviations

ICU: intensive care unit; PCT: procalcitonin.

Competing interests

The authors declare that they have no competing interests.

See related research by Hochreiter et al., http://ccforum.com/content/13/3/R83

Contributor Information

Stephan Harbarth, Email: stephan.harbarth@hcuge.ch.

Werner C Albrich, Email: Werner.Albrich@ksa.ch.

Beat Müller, Email: happy.mueller@unibas.ch.

Acknowledgements

All authors have received speaker honoraria from BRAHMS AG. SH and BM have received research support from BRAHMS AG.

References

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