Critically Ill Clinical Trial
Official title:
Role of Polymorphisms in the Dectin-1 Gene in Determining the Risk of Candida Colonization and Infection in Critically Ill Patients
The principal aim of this study is to establish if a polymorphism in a gene important for innate immunity to fungi represents a significant risk factor for the development of Candida colonisation and subsequent invasive candidosis in critically ill patients. Incorporation of a screening programme onto a risk-based algorithm for critical care patients would allow more effective targeting of molecular diagnostic tests, anti-fungal prophylaxis and targeted treatment. Sequential critical care patients will be screened for gene polymorphisms and undergo regular screening for Candida colonization.
Invasive fungal infections are associated with increased morbidity and mortality rates as
high as 50% (1). Up to half occur in non-neutropenic; critically ill patients and the
majority are due to Candida species. A number of randomised controlled trials (RCTs) have
evaluated anti-fungal prophylaxis, predominantly with fluconazole in critically ill patients
and three systematic reviews of these RCTs have been performed (2-4). Meta-analyses
demonstrated a homogeneous effect of anti-fungal prophylaxis on the risk of proven infection
and some suggested a reduction in mortality. However widespread use of anti-fungal drugs is
expensive, promotes resistance, cause a shift in pathogenic species towards more difficult
to treat infections and may be associated with adverse drug related events. It is necessary
to establish a method to identify patients at greatest risk of fungal infection and thus
those who will benefit most from anti-fungal prophylaxis. Numerous risk factors have been
identified including colonization, class/duration of antibiotics, number/location/duration
of lines, total parenteral nutrition, gastric acid suppression, bacterial sepsis,
post-surgical complications etc, but none accurately predict infection or fungal related
mortality. Given the risk factors for fungal colonisation include infection, sepsis and
antibiotic use, information regarding concomitant antibody deficiency will also be collected
using calculated globulin (part of routine liver function testing) and immunoglobulins.
Recent evidence suggests fungi can modulate and evade host immunity and use surface
molecules coded for by immune response genes that enable them to promote protective
tolerance leading to colonisation and persistence (5). Genetic predisposition to infection
may be associated with polymorphisms in some of these immune response genes. Many of these
polymorphisms relate to a single difference in only one single nucleotide at defined
positions in the DNA sequence. These single nucleotide polymorphisms (SNPs) are common
occurrences within the human genome although frequency can vary markedly according to ethnic
or geographical background. A single SNP may alter both innate and adaptive immunity and
increase the risk of invasive fungal disease.
Dectin-1 is a C-type lectin receptor that plays a central role in host defence against
candidal infection. A common polymorphism in the gene coding for Dectin-1 has been
identified and is associated a functional defect in the immune response and increased risk
of candidal infection (6). Dectin-1 recognizes the ß-1,3-glucan on cell walls and synergizes
with toll-like receptors (TLRs) TLR2 and TLR4 to promote Th1 and Th17 responses to activate
anti-fungal host defence. It is suggested that Dectin-1 has a role in both resistance and
tolerance to fungal infection (7). A polymorphism (Tyr238X) in exon 6 of the Dectin-1 gene,
that results in an early stop codon leading to the loss of the last 10 amino acids of the
extracellular domain, has been identified and leads to diminished binding capacity. This
mutation is thought to be present in around 14% of the population with an allele frequency
of 8% (8). Although data in UK populations are limited, heterozygosity for this mutation has
been linked to recurrent mucocutaneous candidal infection and increased colonization rates
(6). Although no link with invasive disease has been established yet, colonization is a
major risk factor and so a causal link can be postulated. More studies are needed to
investigate this and inform strategies for prophylaxis and pre-emptive anti-fungal
treatment. Screening these patients for Dectin-1 polymorphism will not only investigate
allele frequency in a UK population and provide information on this SNP as a risk factor for
fungal infection but also enable this to be built into a rule-based algorithm that can
identify high-risk patients who would benefit from anti-fungal prophylaxis and/or targeted
molecular diagnostics.
The association between primary or acquired immunodeficiency and susceptibility to fungal
infection has also long been recognised (9)and measurement of antibodies to Candida albicans
have been used as a screening test for humoral immunodeficiency in patients (10).
Perturbations of immunoglobulin levels have not been extensively studied in critically ill
patients. However two small observational studies demonstrated that hypogammaglobulinaemia
was relatively common in patients with septic shock on admission to critical care and was
associated increased mortality (11 12). However, it is unclear whether this is a consequence
of critical illness or a predisposition in some individuals that makes them more susceptible
to critical illness. Calculated globulin (total protein - albumin) forms part of the liver
function tests that are routinely performed in hospital and has been used on an all Wales
basis to screen for previously undiagnosed primary and secondary immunodeficiency.
Calculated globulin can be utilised in the same way to identify patients with low (<18g/dl)
immunoglobulin levels at hospital or critical care admission. Changes in immunoglobulin can
then be tracked throughout critical illness using the calculated globulin and additional
analysis performed in selected patients for more subtle defects in humoral immunity.
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