EDITOR:
Thank you for the opportunity to respond to Dr Mackenzie. Dr Mackenzie is wrong to assert that we ‘considered it more rational to use our cited approach rather than have further formal drug appraisal’. At the time of writing up our collective experience as the five largest UK users of drotrecogin alfa in severe sepsis [Reference Ridley, Lwin and Wyncoll1], very little was known about the use of drotrecogin alfa in routine clinical practice. Moreover, it was far from clear that it was ethically justifiable to perform a further trial, given that the drug has been licensed since 2002 and is currently used in high risk cases around the world. The majority of intensive care units in the UK, and many intensivists now have some experience of using the drug. Use of the drug in the UK has remained constant since early 2006 in spite of the announcement of the new trial (Eli Lilly, personal communication).
In his letter, Dr Mackenzie restates the well-documented views questioning the efficacy of the drug. Many of these arguments have been answered on numerous occasions to the satisfaction of the majority of clinicians, but we accept not all [Reference Laterre2]. However, the fact remains that in appropriately selected cases of severe sepsis at high risk of death [Reference Camporota and Wyncoll3], drotrecogin alfa reduces mortality, which is why both the FDA and EMEA have decided not to withdraw the drug from the market.
Over the last few years there have been an increasing number of audits and registries of the use of drotrecogin alfa in clinical practice which are remarkably consistent, and confirm the results of the original trial [Reference Kubler, Mayner-Zawadzka and Durek4–Reference Beale, Brunkhorst, Martin, Williams, Nelson and Janes6]. In the UK the ICNARC registry of 1245 drotrecogin alfa-treated patients, which used several different ways to match cases (historic admissions, contemporaneous admissions from the same unit, contemporaneous admissions from units that never used drotrecogin alfa, or contemporaneous admissions from units prior to first use), there was not even the remotest signal to harm; in fact, the results were very consistent with the mortality reduction seen in PROWESS [Reference Rowan, Welch, North and Harrison7]. An Italian registry also showed a reduction in mortality but also clearly demonstrated that the drug must be prescribed according to the Summary of Product Characteristics [Reference Bertolini, Rossi, Anghileri, Livigni, Addis and Poole8].
The very low usage that Dr Mackenzie highlights in France [Reference Muller, Jaber, Raillard and Lefrant9] may have more to do with the very cumbersome remuneration mechanism in that country, rather than the view of the clinicians that the drug is not safe.
In summary, we believe the audit we conducted of our earliest use of drotrecogin alfa was valid and responsible, and shows that when used according to the licensed indications is safe and effective in patients with septic shock. We are saddened that Dr Mackenzie feels it is necessary to continue attacking the drug [Reference Mackenzie10–Reference Mackenzie12] rather than adopting a more open-minded and balanced perspective, which might include a description of his own experience with the drug.