Clinical Characteristics and Predictive Factors of Invasive Fungal Disease in Pediatric Oncology Patients with Febrile Neutropenia in a Country with Limited Resources.

BACKGROUND: The most common complication among pediatric oncology patients is febrile neutropenia (FN). Invasive fungal disease (IFD) is suspected when fever persists >4-7 days after empirical antibiotics. Its clinical characteristics and predictive factors associated with IFD among pediatric oncology patients with FN were thus explored.
METHODS: Pediatric oncology patients with FN between January 1, 2012 and December 31, 2016 were enrolled in this study. Clinical characteristics, including laboratory investigations, treatment modalities, and final outcomes of IFD were retrospectively reviewed and analyzed.
RESULTS: In all, 73 patients with 180 episodes of confirmed diagnosis of FN were studied. Median age at diagnosis was 6.2 years, with equal sex distribution. The most common diagnosis was acute lymphoblastic leukemia (n=91, 51%), followed by acute myeloid leukemia (n=47, 26%), Burkitt's lymphoma (n=7, 4%) and neuroblastoma (n=7, 4%). Median absolute neutrophil count at FN diagnosis was 0 (0-806) cells/mm3. IFD was diagnosed for 25 (14%) episodes. Mortality rates for FN and IFD were 4% and 20%, respectively. Respiratory compromise, oxygen requirement, hypotension, prolonged hospitalization, duration of fever and neutropenia, bacteremia, bacteriuria, funguria, abnormal liver-function results, and prolonged broad-spectrum antibiotic administration were factors associated with IFD (P<0.05). Prolonged duration between initiation of fever and antifungal administration for nearly 10 days was an independent factor in prediction of IFD occurrence (P=0.014).
CONCLUSION: Respiratory compromise, oxygen requirement, hypotension, prolonged hospitalization, duration of fever and neutropenia, bacteremia, bacteriuria, funguria, abnormal liver-function results and prolonged broad-spectrum antibiotic administration were factors associated with IFD. Duration between initiation of fever and antifungal administration of nearly 10 days were considered a risk factors of IFD among patients with FN. IRB REFERENCE NUMBER: IRBRTA 825/2560.

Background

The most common complication among pediatric oncology patients is febrile neutropenia (FN). FN is mostly caused by mucocutaneous infection in the gastrointestinal tract, pulmonary system, and skin from bacteria and fungi. Occult bacteremia is found in 20%–30% of patients with FN1 and related to neutropenia of <100 cells/mm3.2 Patients hospitalized for fever and neutropenia are often treated with empirical antibiotics. Investigations and treatment of invasive fungal infection with antifungals is initiated when fever persists >4–7 days or when the patient exhibits illness. A third of these patients are at risk of fungal coinfection, ie, candidiasis or aspergillosis. Clinical symptoms, such as respiratory distress, sinonasal symptoms, and abdominal pain with laboratory such findings as bacteremia or fungemia or funguria,3 may warrant further workup for invasive fungal disease (IFD).

Patients receiving high-intensity chemotherapy regimens are at increased risk of developing IFD. Only 5.8% of patients with FN were ultimately diagnosed with IFD in one high-income country,4 while higher rates up to 23% were found in a country with limited resources.5 Related studies have shown increasing risk of developing IFD correlate with prolonged duration of neutropenia after initiation of fever, treatment of acute myeloid leukemia,6 high-risk (or relapsed) acute lymphoblastic leukemia,7 high-dose steroid exposure,8 prolonged use of empirical antibiotics,9 and pre-existing sites of fungal colonization.10,11 Patients who develop fever during the induction phase of treatment (compared with the maintenance phase) and patients with early fever onset, ie, fever occurring within 5 days of becoming neutropenic appeared to be at higher risk of IFD.12

The mortality rate of FN due to Gram-negative septicemia is 10%–30%,13 while that of Gram positive septicemia is 28%.14 Similarly, the mortality rate of overall IFD is 48.2%.9 Specifically invasive aspergillosis has a mortality rate as high as 30%.15

Most publications had defined IFD using clinical criteria, along with culture or biopsy of involved tissue. However, few of these reports have detailed whether the clinical characteristics, signs and symptoms, laboratory findings, or previous treatment are associated with IFD occurrence.4 Moreover, studies have been conducted in different geographical areas and populations, such as South America4 or adult patients.16 Accordingly, these findings in a pediatric population might be considered as specific guidelines to create greater awareness in center with limited resources, such as in Southeast Asia.

This study primarily aimed to explore clinical characteristics, including investigational and treatment approaches, and associated prognostic factors of IFD, specifically in a pediatric oncology population presenting FN.

Methods

Patient Selection

Medical records of 85 pediatric oncology patients, newly diagnosed and treated for FN primarily at the Division of Hematology and Oncology, Department of Pediatrics, Phramongkutklao Hospital, from January 1, 2012 to December 31, 2016 were retrospectively reviewed.

Inclusion criteria were oncology patients aged 0–21 years whose diagnosis of FN had been confirmed by FN definitions in the 2010 Infectious Disease Society of America clinical practice guidelines.17 Patients with incomplete diagnosis criteria, undergoing hematopoietic stem–cell transplantation (HSCT), or with a previous diagnosis IFD were excluded from the study.

This study was approved by the Institutional Review Board, Royal Thai Army Medical Department according to the ethics principles of the Declaration of Helsinki (1975) and its revisions (IRBRTA 825/2560).

Laboratory Procedure

Galactomannan was detected in serum by direct double-sandwich ELISA, with an index value ≥0.5 considered positive.

Operational Definition of Febrile Neutropenia

Patients had to meet two criteria: fever defined as a single oral temperature measurement >38.3°C (101°F) or >38°C (100.4°F) sustained over 1 hour, and neutropenia defined as an absolute neutrophil count (ANC) <500 cells/mm3 or expected to decline to this level.17

Institutional Definition of Fungal Infections

IFD definition was adapted from the European Organization for Research and Treatment of Cancer (EORTC)–Invasive Fungal Infections Cooperative Group and the National Institute of Allergy and Infectious Diseases Mycoses Study Group (MSG) Consensus Group.18,19

Proven IFD was defined as documented constitutional symptoms with evidence of fungus isolated from normally sterile body fluid or confirmed by histopathology.

Probable IFD was defined as documented constitutional symptoms in appropriate host factors with radiological findings confirmed by a radiologist, ie, computed tomography scan showing dense, well-circumscribed lesions with or without a halo or air-crescent sign, cavities, and evidence of fungus isolated from nonsterile body fluid or laboratory evidence of galactomannan antigen or β-D-glucan detected in serum.

Possible IFD was defined as documented constitutional symptoms in appropriate host factors with no laboratory support in a nonendemic mycosis area.

Mucosal fungal disease was defined as documented symptoms and confirmed histopathology or positive culture of specifically nonsterile mucosa, ie, the skin or esophagus.

Diagnostic Definitions

Respiratory compromise was defined as any symptoms addressing deterioration in respiratory function, ie, use of accessory muscle, and increased or decreased respiratory rate according to age.

Oxygen requirement was defined as abnormal cardiopulmonary conditions causing respiratory compromise that required oxygen therapy to maintain target oxygen saturation >94% in room air.

Hypotension was defined as blood pressure less than the fifth percentile according to age and/or 90/50 mmHg.

Abnormal liver-function test (LFT) results were defined as at least one of increased alanine aminotransferase (ALT), increased aspartate aminotransferase (AST) at least double the upper normal limit, increased total bilirubin concentration, or decreased serum albumin.

Treatment of Febrile Neutropenia

Ceftazidime and amikacin were given to pediatric oncology patients with FN as a first-line empirical antibiotic regimen after blood cultures had been collected. Meropenem would be substituted due to unresponsive treatment. Additionally, vancomycin was considered for patients who were clinically unstable, with possible skin infection or suspected catheter-related infection. Amphotericin B was given as an empirical antifungal if fever had persisted >4–7 days.

Statistical Analysis

Baseline values of demographic data, clinical manifestations, laboratory studies, treatment strategies, and outcomes from all participating patients were analyzed using descriptive statistics and are presented as means ± SD (normal distribution) or medians with range (abnormal distribution) for continuous variables and calculated using frequency and percentage for categorical variables. Categorical and continuous variables were compared using Fisher’s exact and Mann–Whitney U tests, respectively. Univariate and multivariate binary logistic regression analyses were performed to analyze the impact of possible factors on defined outcomes. Five to ten potential risk factors on defined outcomes from observational experience were chosen and analyzed in the univariate analytic model. In addition, all factors that were statistically significant on univariate analysis were also analyzed with multivariate analysis and affirmed interrelationships among several variables. The number of patients was sufficient for an acceptable level of statistical power to perform the multivariate analysis. Statistical analysis was performed using IBM SPSS 23.0, and P<0.05 was considered statistically significant.

Results

Patient Characteristics

Among 85 oncology patients who presented with fever and neutropenia, 12 were excluded due to previously diagnosed confirmation of IFD and inability to confirm clinical criteria of FN. As such, 73 patients with a confirmed diagnosis of FN for a total of 180 FN episodes were subsequently studied, as shown in Figure 1. Patient age, sex, diagnosis, status of disease, and complete blood–count parameters, including initial white blood cell (WBC) count and ANC, at diagnosis of FN are summarized in Table 1.

Figure 1

Study flowchart.

Table 1

Characteristics of Febrile Neutropenia Patients (n=180)

Demographics	NonInvasive Fungal Disease (n=155), n (%)	Invasive Fungal Disease (n=25), n (%)	Total (n=180), n (%)	P
Age at FN diagnosis (years)	6.23 (0–19.8)	7 (0.2–15.63)	6.23 (0–19.8)	0.731
Sex				0.184
Male	78 (50.3)	9 (36)	87 (48.3)
Female	77 (49.7)	16 (64)	93 (51.7)
Diagnosis				0.815
Hematologic malignancy	138 (89)	23 (92)	161 (89.4)
Acute lymphoblastic leukemia	80 (51.6)	11 (44)	91 (50.6)
Acute myeloid leukemia	40 (25.8)	7 (28)	47 (26.1)
Chronic myeloid leukemia	3 (1.9)	1 (4)	4 (2.2)
Burkitt’s lymphoma	4 (2.6)	3 (12)	7 (3.9)
Anaplastic large-cell lymphoma	4 (2.6)	0	4 (2.2)
Diffuse large B–cell lymphoma	5 (3.2)	1 (4)	6 (3.3)
Hodgkin’s lymphoma	2 (1.3)	0	2 (1.1)
Solid tumor	16 (10.3)	2 (8)	18 (10.0)
Neuroblastoma	7 (4.5)	0	7 (3.9)
Osteosarcoma	2 (1.3)	0	2 (1.1)
Rhabdomyosarcoma	2 (1.3)	0	2 (1.1)
Ewing sarcoma	0	1 (4)	1 (0.6)
Other	5 (3.2)	1 (4)	6 (3.3)
Brain tumor	1 (0.7)	0	1 (0.6)
Disease status				0.871
New diagnosis	114 (73.5)	18 (72)	132 (73.3)
Relapsed–refractory	41 (26.5)	7 (28)	48 (26.7)
WBC count at FN diagnosis (cells/mm3)	900 (100–28,900)	600 (0–4,300)	800 (0–28,900)	0.038
ANC at FN diagnosis (cells/mm3)	0 (0–806)	0 (0–340)	0 (0–806)	0.164

Notes: Data presented as medians (range) for continuous variables and n (%) for categorical variables. Comparison between two independent data sets was analyzed using Fisher’s exact or Mann–Whitney U tests (age, WBC, and ANC at FN diagnosis). P<0.05 was considered statistically significant.

Abbreviations: FN, febrile neutropenia; NA, not available; WBC, white blood cell; ANC, absolute neutrophil count.

Among the 180 FN episodes, IFD was diagnosed in 25 (13.9%). Median duration between initiation of fever until diagnosis of IFD was 10 (0–53) days. Overall median age was approximately 6.23 (range, 0–19.8) years, and the male:female ratio was 1:1. The most common diagnosis was hematologic malignancy, totaling 161 (89.4%) FN episodes. A majority were acute lymphoblastic leukemia, followed by acute myeloid leukemia, Burkitt’s lymphoma, diffuse large B–cell lymphoma, chronic myeloid leukemia, anaplastic large-cell lymphoma and Hodgkin’s lymphoma. Solid tumors for 18 (10%) episodes involved neuroblastoma followed by osteosarcoma, rhabdomyosarcoma, and Ewing’s sarcoma.

Disease status was divided into newly diagnosed (132, 73.3%) and relapsed or refractory disease 48 (26.7%).

Median WBC count and ANC at diagnosis of FN were 800 cells/mm3 and 0 cells/mm3, respectively.

Only median initial WBC count at FN diagnosis in patients with IFD (600, range 0–4,300 cells/mm3) was significantly lower than those without (900, range 100–28,900 cells/mm3; P=0.038). Age, sex, diagnosis, disease status, and ANC at FN diagnosis between the non-IFD and IFD groups did not significantly differ.

Pathogens Causing Febrile Neutropenia

Among the 180 FN episodes, pathogens causing FN were identified by histopathology, microbiology, or meeting institutional definition of fungal infections in 71 (39.4%) episodes. The most common organisms were bacteria (39, 54.9%), followed by fungus (31, 43.7%) and virus (one, 1.4%; ).

IFD was identified in 25 (13.9%) of the FN episodes, (). Proven IFD totaled seven (28%) episodes, candidemia four (57.1%), invasive aspergillosis two (28.6%), and combined candidemia and cryptococcal skin infection one (14.3%). Probable and possible IFD were identified for 14 (56%) and four (16%) episodes, respectively. For IFD, six (24%) episodes showed IFD concomitant with bacteremia and eleven (44%) with bacterial infection.

Treatment Outcomes

Over 96% (173 episodes) of patients with FN survived, as shown in Figure 2. Seven (4%) patients died. Five (71.4%) had IFD concomitant with bacterial septicemia and/or hemodynamic instability (septic or spinal shock) causing multiorgan failure. One (14.3%) patient had Neisseria meningitidis encephalitis, and one (14.3%) an unidentified pathogen.

Figure 2

Outcomes of patients with febrile neutropenia associated with invasive fungal disease (n=180).

The overall mortality rate among patients with FN was 4%. Patients with IFD had significantly higher mortality (20%, five of 25) than non-IFD (1.3%, two of 155); (OR 19.125, 95% CI 3.477–105.189; P=0.001).

Clinical and Laboratory Factors Associated with IFD

Signs and symptoms, including compromised respiratory symptoms requiring oxygen therapy, hypotension, prolonged hospitalization and duration of fever, neutropenia, and broad-spectrum antibiotics were influential factors associated with IFD on univariate analysis (P<0.05).Multivariate analysis was subsequently performed, and none was an independent risk factors of IFD (Table 2).

Table 2

Clinical Factors Affecting Clinical Outcomes of Invasive Fungal Disease in Febrile Neutropenia Patients (n=180)

	NonInvasive Fungal Disease (n=155), n (%)	Invasive Fungal Disease (n=25), n (%)	Total (n=180), n (%)	P	Crude OR	95% CI	P	Adjusted OR	95% CI
Respiratory symptoms
No	147 (94.8)	8 (5.2)	155 (86.1)		1
Respiratory compromise	8 (32)	17 (68)	25 (13.9)	0.001	39.047	12.983– 117.435	0.066	92.964	0.741–11,665.336
Oxygen requirement
No	148 (94.9)	8 (5.1)	156 (86.7)		1
Yes	7 (29.2)	17 (70.8)	24 (13.3)	0.001	44.929	14.488–139.329	NA
Blood pressure
Normal	147 (88.6)	19 (11.4)	166 (92.2)		1
Hypotension	8 (57.1)	6 (42.9)	14 (7.8)	0.003	5.803	1.817–18.535	NA
Duration of hospitalization (days)
Mean±SD	27.57±22.13	57.24±31.03	31.69±25.62	<0.001	1.038	1.019–1.058	0.839	0.986	0.861–1.129
Duration of fever (days)
Mean±SD	5.33±5.03	17.12±19.15	6.97±9.36	<0.001	1.134	1.066–1.206	0.134	0.827	0.646–1.06
Duration of neutropenia (days)
Mean±SD	16.5±11.92	22.8±16.53	17.38±12.79	0.027	1.033	1.004–1.064	0.665	0.971	0.848–1.111
Duration of antibiotics (days)
Mean±SD	11.84±5.8	23.88±15.76	13.51±8.93	<0.001	1.171	1.094–1.253	0.39	1.116	0.869–1.432

Notes: Data presented as means ± SD for continuous variables and n (%) for categorical variables. Univariate and multivariate analyses were calculated using logistic regression.P<0.05 was considered statistically significant

Abbreviation: NA, not available.

Abnormal LFT results, bacteremia, bacteriuria, and funguria were statistically significantly associated with occurrence of IFD on univariate analysis (P<0.05, Figure 3), but were not independent risk factors of IFD on multivariate analysis.

Figure 3

Laboratory factors affecting clinical outcomes of invasive fungal disease in febrile neutropenia patients (n=180).

Antibiotics Associated with IFD

All patients received antibiotics for FN treatment. Meropenem and vancomycin were associated with the occurrence of IFD. Patients receiving meropenem were associated with IFD (OR 5.338, 95% CI 2.201–12.947; P<0.001). Similarly, vancomycin was also associated with IFD (OR 9.297, 95% CI 3.568–24.225; P<0.001) as shown in .

Influential Factors Associated with Clinical Outcomes among Patients Receiving Antifungal Treatment

Among 61 (34%) FN cases receiving antifungal treatment, 36 (59%) episodes were non-IFD and 25 (41%) IFD. WBC count and ANC at diagnosis of FN, fever, and neutropenia duration were not significant predictive factors of IFD. Occurrence of IFD among patients with FN presenting abnormal LFT results was significantly higher on univariate analysis(OR 3.556, 95% CI 1.218–10.376; P=0.02). Moreover, longer duration between initiation of fever and antifungal administration was a risk factor associated with IFD. Multivariate analysis was subsequently performed, and affirmed that longer duration (nearly 10 days) between onset of fever and antifungal administration remained an independent risk factor of IFD (adjusted OR 1.201, 95% CI 1.038–1.389; P=0.014), as shown in Table 3.

Table 3

Clinical and Laboratory Factors Associated with Clinical Outcomes of Invasive Fungal Disease in Febrile Neutropenia Patients Who Received Antifungal Treatment (n=61)

	NonInvasive Fungal Disease (n=36), n (%)	Invasive Fungal Disease (n=25), n (%)	P	Crude OR	95% CI	P	Adjusted OR	95% CI
WBC count at FN diagnosis (cells/mm3)
Mean ± SD	1150±1080.87	808±961.3	0.216	1.000	0.999–1.000
ANC at FN diagnosis (cells/mm3)
Mean ± SD	67.22±136.35	45.92±106.09	0.510	0.999	0.994–1.003
Liver-function test
Normal	24 (72.7)	9 (27.3)
Abnormal	12 (42.9)	16 (57.1)	0.020	3.556	1.218–10.376	0.093	3.102	0.828–11.622
Duration of fever (days)
Mean ± SD	9.42±7.35	17.12±19.15	0.062	1.051	0.997–1.108
Duration of neutropenia (days)
Mean ± SD	22.28±10.59	22.8±16.53	0.878	1.003	0.965–1.043
Duration between start of fever and antifungal administration (days)
Mean ± SD	5.33±3.74	9.92±7.25	0.008	1.187	1.045–1.348	0.014	1.201	1.038–1.389

Notes: Data presented as means ± SD for continuous variables and n (%) for categorical variables. Univariate and multivariate analyses were calculated using logistic regression. P<0.05 was considered statistically significant.

Abbreviations: WBC, white blood cell; FN, febrile neutropenia; ANC, absolute neutrophil count.

Discussion

The most common serious complication following pediatric hematology/oncology treatment is FN. It causes high fatality, unnecessarily consumed resources, and prolonged hospitalization. Mortality from FN was higher in low- and middle-income countries — 4% in our study and 5.5% in India20 — than high-income countries, eg, 0.6% in the US.21

Pathogens related to FN are bacteria causing bacteremia and fungal infections. IFD is the crucial cause of morbidity and mortality.22 However, FN is sometimes remains unidentified or labeled “fever of unknown origin”.

The epidemiology of FN-causative organisms depends on the country. Fever of unknown origin in countries with limited resources, as in our study, has been reported as 60% compared to 45% in a developed country.22 In addition, Gram-positive bacteremia dominates in countries widely using central venous catheters23 compared to countries with limited resources, which have a higher percentage of occult Gram-negative bacteremia.20

Risk factors of FN in literature reviews have included type of cancer, intensity of chemotherapy, associated comorbidities,24 duration of neutropenia, length of hospital stay, and previous bacteremia.25

Nevertheless, fungal infection remained the leading cause of mortality, especially among immunocompromised patients experiencing FN. IFD represents one of the serious complications among patients undergoing immunosuppressive therapy or HSCT. IFD occurred at 13.9% in our study. This is similar to a recent finding in Siriraj Hospital, Bangkok, Thailand,16 but higher than studies in South America 8.8%22 and the US (4.9%).26 This higher incidence was possibly affected by the lower use of antifungal prophylaxis in a center with limited resources.

Clinical presentations associated with IFD include sinusitis and abdominal discomfort.5 However, abdominal pain and pneumonia predominated in our study. Nevertheless, respiratory distress, oxygen requirement, and hypotension have been documented as high risk factors of FN in developing serious morbidity.25,27,28 In our study, these factors were associated with IFD on univariate analysis, but not as independent risk factors on multivariate analysis.

The most common pathogens causing IFD in pediatric oncology populations were Candida and Aspergillus infection,7,24 which was likewise found in our study.

The definition of IFD is divided into proven, probable, and possible, as described by the EORTC/MSG Consensus Group.18,19 In countries with limited resources, most IFD cases are classified as probable or possible, rather than proven.6,9 In our study, probable IFD totaled 56%, possible IFD 16%, and proven IFD 28%. The low IFD figure might be due to inaccessibility of tissue biopsies and unidentified fungal cultures in a country with limited resources, such as Thailand.

Risk factors associated with IFD in pediatric oncology previously reported include age, cancer type, duration of fever,4 prolonged neutropenia,8 ANC <500 cells/mm3, and prolonged using of broad-spectrum antimicrobial agents.9,28 These are usually reported among patients with mostly hematologic malignancies in most studies.5,9 In addition, most previous studies on pediatric oncology populations have included nonfever or nonneutropenic cases.26 In our study, cancer types were not associated with IFD. However, our study is one of the few to report both hematologic (90%) and solid malignancies (10%) among children with fever and neutropenia. This variation affected the results differently. In our study, ANC at diagnosis of FN was not associated with IFD. This was because average ANC was 0 cells/mm3 in our study population, regardless of IFD occurrence. ANC in our report was much <500 cells/mm3 which has been documented as an IFD risk in most published data.

We identified bacteremia concomitant with IFD in 24% of patients with IFD. This was possibly because most patients with IFD received multiple and prolonged administration of broad-spectrum antibiotics, such as meropenem and vancomycin, for prolonged fever and neutropenia.29 Antifungal therapy is considered for patients presenting persistent or recurrent fever after 4–7 days of receiving broad-spectrum antibiotics according to Infectious Disease Society of America clinical practice guidelines.17 Therefore, this group of patients is more susceptible to developing multidrug-resistant bacteremia,30 which often leads to the development of systemic coinfection such as bacterial septicemia, urinary tract infection, or enteritis.

Interestingly, abnormal LFT results associated with IFD were found in this study, though not an independent risk factor. Abnormal LFT results might represent an early sign of organ compromise or septicemia, which are risks factors of developing IFD.

In summary, the abnormal LFT results, bacteremia,3,29,31 bacteriuria, and funguria found in our study were associated with IFD.

On multivariate analysis, patients with IFD had significantly longer duration, nearly 10 days, between initiation of fever and antifungal administration than patients without IFD. This presumably prolonged waiting period for antifungal administration was associated with developing IFD. Earlier administration of antifungal treatment could be a potential factor in suppressing IFD manifestation in patients with FN. As such, this finding was not truly an independent predictive factor of IFD. However, if patients experience symptoms suspected to be IFD and fever >4–7 days after empirical antibiotics, antifungal treatment should be considered promptly and not postponed >10 days.

The mortality rate of IFD was 20% in our study, similar to 25% in Taiwan15 and 14%–29% in US studies,26,32 whereas antifungal prophylaxis was widely used. The causes of death are associated with concomitant bacterial septicemia causing multiorgan failure.

To our knowledge, this study is the first to identify predictive factors of IFD in a Southeast Asian pediatric oncology population with FN.

Limitations

This was a retrospective study on IFD that was mostly “probable” or “possible” by definition, and thus does not represent a study of an entire group of IFD cases that should otherwise be diagnosed by proven IFD. Moreover, all patients with IFD in our study were in fever and neutropenic settings. We excluded patients with IFD undergoing HSCT and presenting nonfever and nonneutropenic IFD,7 which would have represented an entire population of patients with IFD.

Conclusion

This study affirmed that IFD was the main factor contributing to the high mortality rate among pediatric hematology/oncology patients with FN. IFD definitions often meet “probable” or “possible” rather than “proven” cases in countries with limited resources. Addressing the factors associated with IFD is warranted in order to decrease disease mortality and complications. Respiratory compromise, oxygen requirement, hypotension, prolonged hospitalization, duration of fever and neutropenia, bacteremia, bacteriuria, funguria, abnormal LFT results, and broad-spectrum antibiotic administration were factors associated with IFD. ANC was not associated with IFD when <100 cells/mm3. In addition, duration between initiation of fever and antifungal administration of nearly 10 days was a potential influential factor to predict occurrence of IFD, though, earlier administration of antifungal treatment would be a confounding factor suppressing IFD manifestation among pediatric oncology patients with FN.