Selective decontamination of the digestive tract in critical care: a teenage angst or coming of age issue?
Cuthbertson Critical Care
(2018) 22:296
https://doi.org/10.1186/s13054-018-2227-2
EDITORIAL
Open Access
Selective decontamination of the digestive
tract in critical care: a teenage angst or
coming of age issue?
Brian H. Cuthbertson
See related research by de Jonge et al., https://ccforum.biomedcentral.com/articles/10.1186/s13054-018-2170-2
Abstract
Selective decontamination of the digestive tract (SDD)
has been with us since the early days of our specialty,
and in some ways it marks our progression and
maturation. How we have dealt with SDD to date
ranges from “thorn in our side” to “elephant in
the room”. With high quality multi-national studies
underway, how we deal with these results will mark
our final maturation to adulthood as a specialty.
Keywords: Sepsis, Prevention, Selective
decontamination of the digestive tract, Antibiotics,
Evidence
It is said that that there are several ages of man: infancy,
adolescence, coming of age, adulthood and senility or as
Douglas Adams stated Survival, Inquiry and Sophistication, otherwise known as the How, Why and Where
phases [1]. It could be suggested that the stages of man
have their analogies for a medical specialty, and if this
holds true, then intensive care medicine should surely be
passing from its coming of age stage into adulthood at
this time in its development. Since selective decontamination of the digestive tract (SDD) has been with us
through all stages to date, perhaps how we deal with this
issue is a litmus test of whether we have indeed reached
adulthood as a profession.
Back in the 80s, when SDD first came to eminence (or
was it notoriety), we were still an infant specialty. At this
time, we correctly identified that sepsis was “our disease”
and we needed to be better at both preventing and treating it to save more lives. This led to the suggestion that
Correspondence:
Department of Critical Care Medicine, Sunnybrook Health Sciences Centre,
University of Toronto, Toronto M4N 3M5, Canada
using topical antibiotics to selectively target Gramnegative aerobic bacteria in the gut (the cause of the majority of hospital-acquired infections at that time) could
prevent sepsis; from this SDD was borne [2]. Since then
there has been over 37 randomised controlled trials
(RCTs) and 12 meta-analyses (more meta-analyses than
many topic areas have individual RCTs) [3]. In brief,
these meta-analyses suggest that an SDD regimen that
includes an intra-venous antibiotic saves lives and prevents ventilator associated pneumonia (VAP) in the critically ill [3]. Further, meta-analysis of the (mostly
inadequate) antibiotic resistance data arising from these
RCTs suggests that SDD may have no effect, or potentially reduce antibiotic usage and antibiotic resistance
rates [4]. Despite this, detailed surveys and studies of
barriers to implementation show that a large number of
centres around the world have neither implemented
SDD into their practice nor intend to do so [5]. The reasons quoted for this stance ranged from considered and
reasonable (“I am concerned about antibiotic resistance”)
to extra-scientific (“there is no supportive evidence” and
“in order to adopt SDD in my unit someone would have
to assassinate me”), with extra-scientific in this context
clearly being a gentle euphemism for biased [6].
So why does SDD bring about such strong reactions
amongst our profession and why has there been so little
implementation of this strategy into our practices? There
is no question that rising antibiotic resistance rates now
threaten our ability to treat infections with antibiotics.
There is also little doubt that, despite the large number
of RCTs in this field, the age and spectrum of methodological quality of these RCTs makes the strength of evidence less than conclusive [3]. Further, with the
implementation of various strategies to reduce infectious
complications in critical care, the contemporary relevance of this evidence base may also be in doubt. If
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Cuthbertson Critical Care
(2018) 22:296
these were the reasons by which we had conscientiously
and considerately declined to implement SDD into our
practice, we would be largely justified; but there is more
to this story. The evidence would suggest that our biases
towards SDD may have clouded our judgement [6]. We
could argue that we are a conservative specialty that appropriately awaits rigorous evidence before considering
clinical implementation; and that would be laudable if it
were true. However, as a profession we have implemented other treatments with far less supportive evidence, including the widespread implementation of
steroids in septic shock after a small RCT of moderate
quality [7, 8]; the promotion and implementation of
chlorhexidine mouthwash for VAP in general critical
care populations by various governmental and nongovernmental bodies despite a weak to moderate evidence base coming mostly from trials in cardiac surgery
patients [9]; the promotion and widespread implementation of tight glycaemic control despite the evidence coming from one single centre RCT of moderate quality
[10]. All of these areas were succeeded by higher quality
evidence that demonstrated that these treatments were
either harmful or at least non-beneficial [11–13]. Not so
conservative, it would seem!
So, returning to our analogy, these examples seem to
show the teenage angst of our profession as we struggle
to deal with developing, and at times contradictory, evidence bases. Going forward we need to deal with evolving evidence bases in a more considered fashion,
including a more considered approach to guideline development and more conservative and rigorous implementation strategies. Coming back to SDD, large,
high-quality, multi-national trials are currently underway
testing the role of SDD in preventing deaths from sepsis
whilst also studying the trade-off effects of SDD on antibiotic resistance [14, 15]. It does seem reasonable to
hold any further implementation of SDD whilst these
trials are completed.
Conclusion
How we deal with the ultimate results of these SDD
studies will act as the litmus test of whether we, as a
specialty, have come of age.
Abbreviations
RCT: Randomised controlled trials; SDD: Selective decontamination of the
digestive tract; VAP: Ventilator associated pneumonias
Acknowledgements
I have no acknowledgements.
Funding
There was no funding for this article.
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