Ethics

This observational study was based on anonymized hospitalization reports and was in strict compliance with the reference methodology MR-004 of France. The study was approved by the data protection authority, Commission Nationale de l’Informatique et des Libertés (registration no. 2220799v0), and received a favorable opinion from the Comité Ethique de la Société de Réanimation de Langue Française institutional review board (approval no. 20–95). The study was conducted in accordance with principles of the Declaration of Helsinki (World Medical Association, https://www.wma.net).

Study Population

We retrospectively included in the study adult ICU patients with a diagnosis of invasive fusariosis during January 1, 2002–December 31, 2020. We used a modified EORTC/MSG criteria to determine diagnosis of proven or probable invasive fusariosis (7) (Appendix Table 1). We identified patients by reviewing medical records, microbiologic databases, or both. To identify patients eligible for our study, we conducted a comprehensive screening of all ICUs and parasitology and mycology departments in France from which Fusarium species had been identified. Of 47 screened ICUs, only 16 had patients with a positive Fusarium microbiologic documentation during the inclusion period. We assessed a total of 120 patients for eligibility. We excluded 53 patients with Fusarium colonization and ultimately included 55 patients in the study (Figure 1).

We collected data from anonymized hospitalization reports, including information on patient age, sex, underlying disease conditions, history of immunodeficiency, clinical and microbiologic characteristics of the Fusarium infection, any co-infections, antifungal treatment, need for organ support, and outcomes. For each patient, simplified acute physiology score (SAPS II) and sequential organ failure assessment (SOFA) scores were collected at admission, as previously defined (20,21). For response to therapy, we defined progression as clinical deterioration or death after antifungal treatment. We considered response complete if clinical improvement occurred, biological samples became sterile, and computed tomography (CT) features cleared. When all the complete response criteria were not met, we considered response to therapy to be partial.

Outcomes

Our primary objective was to identify factors associated with ICU mortality rates. Our secondary objective was to identify factors associated with response to therapy.

Statistical Analyses

We reported continuous variables as medians and interquartile ranges (IQRs) and categorical variables as numbers and percentages. We considered response to treatment, death in the ICU, death in the hospital, and death within 1 year as binary endpoints for the main analysis. We compared continuous variables by using Wilcoxon rank-sum test and compared categorical variables by using Fisher exact test. We performed adjusted analyses to evaluate factors associated with treatment response and death by using multivariable logistic regression models. We estimated cumulative incidence of death in the ICU by using standard methods for competing events and considered discharged alive as a competing outcome to ICU death. We performed all tests 2-sided at the 5% significance level. We performed all analyses on the R statistical platform (The R Foundation for Statistical Computing, https://www.r-project.org).

Patient Characteristics

We identified 55 patients with invasive fusariosis in 16 ICUs during the inclusion period (Table 1). The median age was 61 (IQR 52­–67) years; 80% (n = 44) were immunocompromised, most (n = 32) of whom had active hematologic malignancies (36%, n = 16) or underwent a recent (<1 year) allogeneic hematopoietic stem cell transplantation (allo-HSCT) (36%, n = 16). Eleven (25%) immunocompromised patients had a medical history of solid organ transplantation. Of 11 (20%) immunocompetent patients, all had invasive fusariosis diagnosed during a prolonged (>2 weeks) ICU hospitalization, including hospitalization for septic shock (n = 7), acute respiratory distress syndrome (n = 2), and multiple traumatic injuries (n = 2). Only 24% (n = 13) of patients had an antifungal prophylaxis at ICU admission. Patients admitted to the ICU had severe illness as indicated by elevated median SAPS II and SOFA scores.

During ICU stays, acute respiratory failure was the main organ failure in patients with invasive fusariosis; 80% (n = 44) of patients required invasive mechanical ventilation (Table 2). Furthermore, acute kidney injury was observed in 73% (n = 40) of patients, among whom 29 (72.5%) required renal-replacement therapy, such as continuous venovenous hemofiltration and hemodialysis. The incidence of acute kidney injury was notably higher (100%) for the 11 patients with solid organ transplant than for the patients with hematologic malignancies (44%, n = 7), allo-HSCT (69%, n = 11), and other patients (92%, n = 11) (p = 0.003) (Appendix Table 2).

Patients experienced prolonged ICU hospitalizations; median length of stay was 17 (IQR 6­–37) days, and the mortality rate was high (56%, n = 31). Of 31 ICU patients who died, 18 (58.1%) deaths were considered directly related to invasive fusariosis and 13 (41.9%) deaths were not considered directly related to invasive fusariosis. Of those 13 deaths, causes were multivisceral organ failures related to secondary infections (n = 6), severe graft versus host disease (n = 1), progression of the underlying malignancy (n = 2), hemorrhagic shock (n = 1), or withdrawal of life-sustaining treatment (n = 3). Among ICU survivors, 1 (4%) patient died in the hospital and 3 (4%) patients died within 1 year of diagnosis.

Invasive Fusariosis in ICUs

Using EORTC/MSG criteria, we classified a total of 32 (58%) cases as probable invasive fusariosis and 23 cases (42%) as proven invasive fusariosis (Table 3). Among invasive fusariosis patients, 53% of diagnoses were established after admission to the ICU; median time from ICU admission to invasive fusariosis diagnosis was 9 (IQR 1–16) days. Mycologic diagnosis was achieved through culture of various biologic samples and was guided by the patients’ clinical signs and symptoms. Blood cultures (22%, n = 12) were used for cases of fever and disseminated invasive fusariosis, biopsies (29%, n = 10) were taken from skin lesions, sputum (29%, n = 16) and bronchoalveolar lavage fluid (22%, n = 12) were collected for pneumonia cases, sinus aspirate samples (5%, n = 3) were obtained for sinusitis, joint fluid (5%, n = 3) was examined for arthritis, and pancreatic fluid (2%, n = 1) collections were analyzed for suspected infection (Figure 2). Pathologic examination of skin or sinus biopsies revealed Fusarium associated with tissue damage in 10 (18%) patients.

Results of serum galactomannan test were available for 50 (90.9%) patients and 15 (30%) of them had a positive serum galactomannan test on the day of invasive fusariosis diagnosis. Among those patients, 4 also had concomitant aspergillosis diagnosed. Other observed co-infections included bacterial co-infection in 58% (n = 32), viral co-infection in 35% (n = 19), and fungal co-infection in 34% (n = 19) of invasive fusariosis patients (Appendix Table 3).

Pneumonia was the most prevalent clinical manifestation, accounting for 76% (n = 42) of the cases. Consistent with the EORTC/MSG criteria, the diagnosis of fungal lung disease primarily relied on thoracic CT. Among the patients, fusariosis-related pneumonia exhibited a wide range of thoracic CT patterns (Figure 3): 43% (n = 16) had pulmonary consolidations, 32% (n = 12) had nodules and micronodules, 24% (n = 9) had ground glass opacities, 16% (n = 6) had pleural effusion, and 8% (n = 3) had excavated pulmonary lesions. Moreover, the incidence of disseminated invasive fusariosis was notably higher (44%, n = 7) in patients with hematologic malignancies than in patients who had allo-HSCT (25%, n = 4) or solid organ transplants (9%, n = 1) (p = 0.03) (Appendix Table 2).

Two thirds of invasive fusariosis patients received antifungal monotherapy. The 2 primary drugs used were voriconazole (62%, n = 34) and amphotericin B (60%, n = 33). Four (7%) patients died before invasive fusariosis diagnosis and did not receive treatment. Granulocyte colony-stimulating factor was administered to 55% (n = 12) of the neutropenic patients, and surgical debridement of localized lesions was performed in 13% (n = 7) of patients. Half of the patients experienced disease progression despite receiving adequate therapy.

Factors Associated with Response to Therapy

Factors associated with invasive fusariosis progression under therapy in all 55 patients by univariate analysis were history of recent (<1 year) and past (>1 year) allo-HSCT (p = 0.049), corticosteroid therapy for >3 weeks (p = 0.019), a higher SOFA score at admission (p = 0.002), performance status >2 at admission (p = 0.022), and pulmonary consolidations on thoracic CT for fusariosis-related pneumonia (p = 0.001) (Appendix Table 4). Conversely, nodules and micronodules on thoracic CT were significantly associated with partial and complete response (p = 0.001). By multivariate analysis, none of the following were significantly associated with response to therapy: voriconazole treatment (odds ratio [OR] 3.55, 95% CI 0.72–17.6; p = 0.12), history of allo-HSCT (OR 0.21, 95% CI 0.036–1.24; p = 0.086), and disseminated fusariosis (OR 0.15, 95% CI 0.015–1.42; p = 0.098).

Factors Associated with Death

By univariate analysis, signs and symptoms significantly associated with death in the ICU included history of hematologic malignancies and allo-HSCT (p = 0.017), immunosuppressive therapy other than corticosteroids (p = 0.036), elevated SAPS II (p = 0.007) or SOFA (p = 0.001) score at admission, and neutropenia (neutrophils <0.5 G/L) (p = 0.05) (Appendix Table 5). Among patients with organ failure, only vasopressors were associated with death (p = 0.006). Conversely, surgical debridement of localized lesion was associated with ICU survival (p = 0.014).

By multivariate analysis, the factors associated with death in the ICU were higher SOFA score (OR 1.51, 95% CI 1.15–1.98; p = 0.003) and history of hematologic malignancy or allo-HSCT (OR 8.28, 95% CI 1.26–54.2; p = 0.027). Cumulative incidence of ICU death showed a 50% (95% CI 31.4%–66%) ICU mortality rate at 28 days for patients with hematologic malignancies or allo-HSCT compared with 26.1% (95% CI 10.3%–45.3%) for patients without hematologic malignancy and allo-HSCT (Figure 4). Multivariate analyses on factors associated with death in the hospital and within 1 year of admission were similar to the results of the analyses for factors associated with death in the ICU. Indeed, higher SOFA score was associated with death in the hospital (OR 1.50, 95% CI 1.14–1.97; p = 0.004), death within 1 year of admission (OR 1.66 95% CI 1.16–2.36; p = 0.005), history of hematologic malignancy (OR 7.87, 95% CI 1.18–52.6; p = 0.033 ), or allo-HSCT (OR 15.3, 95% CI 1.60–145.7; p = 0.018).