Comparison of the incidence, clinical features and outcomes of invasive candidiasis in children and neonates

Invasive candidiasis included candidemia and deep-seated candidiasis, which were defined as the recovery of a Candida species from blood or a sterile site, respectively [24, 25]. An episode of candidemia was considered to be catheter-related only if the catheter tip culture was positive for the same Candida spp. [26]. Episodes were considered to be separate if they occurred ≥1 month apart. Breakthrough invasive fungal disease was defined as candidemia or positive Candida spp. isolated from a sterile site in a patient who had undergone therapy or prophylaxis with any systemic antifungal drug for ≥3 consecutive days before the index blood culture [8, 27]. Invasive candidiasis-attributable mortality was defined when the patient died within 7 days after onset of invasive candidiasis or in the presence of persistent clinical sepsis or persistent candidemia, or if the patient died of candidemia associated complications [27, 28]. Combined with the antifungal susceptibility results, treatment failure was defined as an infection that led to attributable mortality or cases of persistent candidemia ≥7 days after initiation of effective antifungal therapy. Patient responses to antifungal therapy following invasive candidiasis were defined according to the consensus criteria of the Mycoses Study Group and the European Organization for Research and Treatment of Cancer [29].

Clinical data were analyzed using SPSS version 18.0 (SPSS Inc., Chicago, IL, USA). Variables associated with invasive candidiasis in the NICU were compared with non-neonatal episodes. Univariate analyses were performed using Student’s t-test or non-parametric tests as appropriate (for continuous variables) or the chi-square or Fisher’s exact tests (for categorical variables). All tests were 2-tailed, and a P value of < 0.05 was considered significant. We performed multiple logistic regression analyses to identify clinical risk factors that were associated with treatment failure of invasive candidiasis. All risk factors that were significant at 0.10 in the univariate analysis were included in the corresponding multivariate analysis.

Invasive candidiasis occurred in 152 boys (54.1% of all patients) and 129 girls. The mean age for non-neonatal pediatric patients was 6.2 ± 5.7 years (range, 3 months to 18 years). Overall, 214 (62.6%) episodes of invasive candidiasis occurred in children ≤3 years old (Fig. 1). Most of the invasive candidiasis episodes were primary bloodstream infections (228 episodes, 66.7%), followed by catheter-related bloodstream infections (69 episodes, 20.2%), and intra-abdominal infections (31 episodes, 9.1%). The sites of isolation and Candida species distributions were not significantly different between the neonatal and non-neonatal groups (Table 1), except that only two episodes in the NICU were caused by C. tropicalis. C. albicans was the most common Candida species that caused invasive candidiasis in children (45.3%, 155 episodes), followed by C. parapsilosis (27.8%, 95 episodes), C. tropicalis (6.4%, 22 episodes) and C. glabrata (6.1%, 21 episodes). Polyfungal isolates (i.e., two different Candida species yielded on cultures of blood samples that were obtained simultaneously) were recovered from three episodes, and the majority of ascites cultures (in 23 episodes, 74.2%) were polymicrobial isolates that also yielded gram-positive cocci, or aerobic and anaerobic gram-negative bacilli.

The majority of patients had multiple underlying illnesses and other risk factors that have been associated with invasive candidiasis (Table 2). The majority of neonatal invasive candidiasis cases occurred in very low birth weight infants (birth weight < 1500 g) (98 episodes, 86.7%), and the mean (SD) gestational age in this group was 27.8 ± 3.9 weeks. The most common predisposing factors were use of central intravenous catheter (CVC) (94.2%), use of broad-spectrum antibiotics (91.8%), stay in an ICU (69.3%), receipt of parenteral nutrition (64.6%), and underlying neurological sequelae (36.0%). For 282 episodes (82.4%), ≥ 4 risk factors and/or underlying illness were identified. However, the underlying illness and major predisposing factors were significantly different between neonatal invasive candidiasis and non-neonatal pediatric episodes. While neonates with invasive candidiasis were significantly more likely to have chronic lung disease and receive total parenteral nutrition, non-neonatal pediatric candidemia were more likely to occur in children with underlying neurological sequelae, cancer treated immunosuppressive agents, neutropenia and artificial devices other than CVC.

No patient developed endophthalmitis, endocarditis, or osteomyelitis that was clinically evident, but five had CNS infection and four had an obstructing renal fungus ball during the follow-up period. In addition, 31 had intraabdominal abscesses or peritonitis and four patients had positive Candida isolates from pleural fluids. 36.8% of invasive candidiasis presented with severe sepsis, and 26.0% had septic shock at the onset of sepsis. After effective antifungal treatment, 17.8% had progressive and deteriorated candidiasis, and 14 (4.1%) had disseminated candidiasis. Neonates with invasive candidiasis had significantly higher severity of illness than children based on the surrogate marker of severe sepsis and septic shock (Table 3).

More than half of the episodes (180 episodes, 52.6%) were characterized by fungemia or persistent invasive candidiasis of > 1 day’s duration, whereas 165 (48.2%) and 78 (22.8%) were characterized by fungemia or persistent invasive candidiasis of ≥3 days and ≥ 7 days, respectively. The mean duration of fungemia was 4.4 days (± 6.2 days). The longest duration of fungemia was 34 days, which occurred in a patient who had end-stage renal disease and who received long term hemodialysis.

Of the 342 episodes, 332 (97.1%) were treated with an antifungal agent, and there were 41 episodes of breakthrough invasive candidiasis. Ten episodes (2.9%) were not treated because of the patient’s death before or at the time of the diagnosis was established. Antifungal therapy was initiated after a mean of 1.81 days (range, 0–6) following the acquisition of the first diagnostic blood and/or sterile site culture and was significantly later in neonates than in children (2.1 ± 1.3 vs. 1.7 ± 1.4 days, P = 0.009). The mean duration of all antifungal therapy per episode was 18.5 days (range, 1–68). Of those 332 episodes for which an antifungal agent was used, 151 episodes (45.5%) had modification of the antifungal regimens during the treatment course, mainly due to the patient’s poor response to initial antifungal therapy (101 episodes, 66.9%), suspicious antifungal resistance after confirmation of Candida spp.(36 episodes, 23.8%), or no reason was documented (14 episodes, 9.3%). Among the antifungal regimens for treatment, fluconazole was the most commonly prescribed initially (62.3%), followed by amphotericin B (24.7%) and caspofungin (4.5%). However, the final treatment regimens were fluconazole/Voriconazole (39.5%), amphotericin B (29.2%) and echinocandin (28.9%), with significant differences between neonates and children (Table 3).

Catheter removal was done within 3 days after illness onset in only one-third of patients with invasive candidiasis (107 episodes, 32.2%), and in 22 episodes, the candidemia resolved only after removal of the intravenous catheter. Neonates with invasive candidiasis had a longer period of fungemia than children, and a higher rate of treatment failure was also noted (31.0% vs. 19.7%, P = 0.015) (Table 3). Invasive candidiasis in neonates was associated with a significantly higher rate of sepsis-attributable mortality than that in children (28.3% vs. 17.5%, P = 0.024). After invasive candidiasis, neonates had a higher rate of in-hospital mortality than children (42.7% vs. 25.4%, P = 0.004, and P = 0.005 by log rank test [Fig. 2]).

In vitro susceptibility to various commonly prescribed antifungal agents in our hospital was determined for 295 isolates (Table 4). The rate of fluconazole-R or S-DD Candida was 14.6% (43 of 295 isolates) overall. The antifungal susceptibility profiles of Candida spp. in neonates were not significantly different between those in non-neonatal pediatric episodes. No trend toward higher minimum inhibitory concentrations was noted when earlier isolates (i.e., isolates recovered during 2004–2009) were compared with those obtained later (i.e., those recovered during 2010–2015).

Except for underlying renal failure that required hemodialysis, none of underlying chronic comorbidities were associated with treatment failure. Treatment failure was not associated with any specific Candida species that caused invasive candidiasis. After multivariate logistic regression analysis (Table 5), the independent risk factors for treatment failure of invasive candidiasis included septic shock (odds ratio [OR]: 16.01; 95% confidence interval [CI]: 7.64–33.56; P <  0.001), delayed removal of intravenous catheter (after 3 days of disease onset) (OR: 6.78; 95% CI: 2.48–18.52; P <  0.001), underlying renal failure with/without hemodialysis (OR: 5.38; 95% CI: 1.99–14.57; P = 0.001), and breakthrough invasive candidiasis (OR: 2.99; 95% CI: 1.04–8.67; P = 0.043).