DOI: 10.1097/01.CCM.0000267653.72988.21
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PMID: 17522532
Issn Print: 0090-3493
Publication Date: 2007/06/01
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Excerpt
PROWESS included patients with severe sepsis and an a priori plan for a primary analysis stratified by a variety of clinical factors (3). Presumably, this would guide subsequent studies, should there be no overall effect. However, there was a mortality benefit for the whole cohort (absolute risk reduction, 6.1%; 95% confidence interval [CI], 1.9–10.3%). After analyzing subgroups, regulatory bodies concluded that the sickest patients benefited the most, and rhAPC was approved for those at a high risk for death. Statistically, an Acute Physiology and Chronic Health Evaluation (APACHE) II score ≥25 provided the best discrimination of those likely to benefit (absolute risk reduction, 12.8%; 95% CI, 6.2–19.4%) (4).
ADDRESS was designed to answer the question about lower-risk patients for whom rhAPC was not already indicated (2). This study was stopped early because of a projected lack of effect. Among ADDRESS patients with an APACHE II score ≥25 (12% of those enrolled), those treated with rhAPC had numerically higher mortality than those assigned to placebo (absolute risk increase, 4.8%; 95% CI, 4.9% decrease to 14.2% increase). This raised questions about PROWESS’ conclusions, despite the clear differences in studies, as shown by the dissimilarity in mortality among placebo patients (APACHE II ≥25: PROWESS = 43.7%, ADDRESS = 24.7%; APACHE II <25: PROWESS = 19.0%, ADDRESS = 16.0%).
The sequence in which we received data produced some of the uncertainty about rhAPC. PROWESS demonstrated a benefit, but only for half of the subjects. Then, ADDRESS showed no effect. We tend to simplify these results as contradictory: one was positive, and one was negative. If the sequence was changed, would the same conclusions have been reached? If PROWESS was without overall effect but the subgroup at highest risk showed a benefit, there would have been a second study examining only those at a higher risk. If that study demonstrated rhAPC was beneficial, we would have reached a consensus that rhAPC should be used for severe septic patients at a high risk for death. Instead, rhAPC has become contentious (5–8).
Given the heterogeneity of severe sepsis, it would be surprising if any single agent were uniformly effective. We certainly would not expect a single chemotherapeutic agent to be useful in all cancers. If a single drug were to be successful, it would have to address pathways common to the majority of patients. Alternatively, it may work only in a subgroup of patients with the targeted derangement. rhAPC may fit such a description. Considering the acceptance of other therapies without definitive mechanisms of action (e.g., lower tidal volume ventilation [9]), it is peculiar that similar uncertainty causes a reluctance to use rhAPC.
The increased risk of bleeding is important when considering rhAPC use. This is a complex issue because we cannot confidently predict who will benefit from treatment and who will bleed.
