Incidence and outcome of invasive candidiasis in intensive care units (ICUs) in Europe: results of the EUCANDICU project

The sample size was of 46 observations (2 for each of the 23 participating ICUs, one in 2015 and one in 2016). Non-independence was accounted by adding center as random effect. The model also included an interaction term (year of study × type of ICU), with p for interaction 0.761. Results of the main model (including both candidemia and IAC) were confirmed in a subgroup analysis including only patients with candidemia and not IAC (n = 422), suggesting that the observed increased cumulative incidence of IC in medical ICU vs. surgical ICU was mainly due to candidemia and not IAC: year of study (CIR 1.09, 95% CI 0.77–1.55, p 0.619), type of ward (p 0.005, with CIR 0.03 for surgical vs. medical, 95% CI 0.00–0.31, and CIR 0.34 for mixed vs. medical, 95% CI 0.07–1.55), year of study × type of ward (p for interaction 0.782), center as random intercept (standard deviation of the random effect = 1.410; model β₀ = − 3.937). Results of the subgroup analysis of patients with IAC (n = 148) were as follows: year of study (CIR 1.77, 95% CI 0.79–4.21, p 0.177), type of ward (p 0.798, with CIR 0.94 for surgical vs. medical, 95% CI 0.07–12.51, and CIR 0.82 for mixed vs. medical, 95% CI 0.12–5.37), year of study × type of ward (p for interaction 0.290), center as random intercept (standard deviation of the random effect = 1.565; model β₀ = − 6.285). Stratified cumulative incidences for countries in the entire study period was as follows: Italy (2 medical and 7 mixed ICUs), 89.62 episodes per 1000 ICU admissions (range 1.20–114.21); France (2 surgical, 1 medical, and 1 mixed ICUs), 11.85 episodes per 1000 ICU admissions (range 0.62–27.63); Greece (1 medical and 1 mixed ICUs), 30.79 per 1000 ICU admissions (range 7.50–45.73); Belgium (1 medical ICU), 9.28 episodes per 1000 ICU admissions; Czech Republic (1 surgical ICU), 0.90 per 1000 ICU admissions; Germany (1 mixed ICU), 42.43 episodes per 1000 hospital admissions; Ireland (1 mixed ICU), 5.63 episodes per 1000 ICU admissions; Portugal (1 mixed ICU), 9.33 episodes per 1000 ICU admissions; Spain (1 mixed ICU), 10.46 episodes per 1000 ICU admissions; The Netherlands (1 mixed ICU), 2.29 episodes per 1000 ICU admissions; UK (1 mixed ICU), 41.67 episodes per 1000 ICU admissions

CI confidence intervals, CIR cumulative incidence ratio, IC invasive candidiasis, ICU intensive care unit, IQR interquartile range

*The model also includes center as a random intercept (standard deviation of the random effect = 1.293; model β₀ = − 3.763)

^§p = 0.022 for the subgroup comparison surgical vs. medical

Results are presented as n (%) unless otherwise indicated. AKI acute kidney injury, COPD chronic obstructive pulmonary disease, CVC central venous catheter, IC invasive candidiasis, IAC intra-abdominal candidiasis, ICU intensive care unit, IQR interquartile range, SAPS simplified acute physiology score, SOFA sequential organ failure assessment, WBC white blood cells

*Only results for variables retained in the final multivariable model (model A) are presented. Variables included in model A were also included in an additional generalized linear multivariable mixed logistic regression model with center as a random intercept (model B; standard deviation of the random effect = 0.311; model β₀ = −4.329), the results of which were in line with those of model A: age (OR 1.04, 95% CI 1.02–1.06, p < 0.001); end-stage chronic renal disease (OR 1.83, 95% IC 0.95–3.52, p 0.070), severe liver failure (OR 3.41, 95% CI 1.33–8.73, p 0.010); previous antibacterial therapy (OR 1.51, 95% CI 0.86–2.63, p 0.148); SOFA score (OR 1.11, 95% CI 1.04–1.18, p 0.001); septic shock (OR 2.09, 95% CI 1.21–3.62, p 0.008), adequate source control within 24 h (OR 0.64, 95% CI 0.38–1.08, p 0.095). The Akaike information criterion (AIC) values for model A and model B were 391.1 and 392.5, respectively

**At the onset of signs and symptoms of IC

***The present exploratory model was not developed to comprehensively assess the overall impact of antifungal therapy and/or adequate source control (including those performed beyond 24 h after the onset of symptoms), which needs further dedicated investigation to be reliably evaluated

^§ClCr < 60 mL/min

^§§C. glabrata (n = 52), C. parapsilosis (n = 38), C. tropicalis (n = 18), C. krusei (n = 14), C. dubliniensis (n = 4), other species with lower frequency (n = 5), more than one non-Candida albicans spp. concomitantly (n = 10)

^§§§C. albicans plus C. glabrata (n = 16), C. albicans plus C. parapsilosis (n = 4), other combinations with lower frequency (n = 7)

^aSevere hepatic failure was defined as liver cirrhosis according to histology or in the presence of a clinical diagnosis supported by laboratory, endoscopy, and radiologic findings

^bSeptic shock was defined as hypotension not responding to fluid therapy and requiring vasoactive agents

^cInformation available (i.e., fluconazole tested) for 274/330 patients (83%)

^dSource control was considered adequate in the following cases: (i) not necessary, (ii) devices or foreign body removal, (iii) drainage of infected fluid collections, (iv) debridement of infected solid tissue, and (v) definitive measures to correct anatomic derangements resulting in ongoing microbial contamination

^eFrom the onset of signs and symptoms of IC. Empiric treatment was considered adequate when the infecting organism was ultimately shown to be susceptible to the empirically administered antifungal. This analysis was conducted in the subgroup of patients not receiving empirical antifungal or receiving empirical antifungals for treating Candida spp. for which susceptibility test results were subsequently available (257/330, 78%)