Highlights
1. Antifungal treatment was associated with a 69% reduction in 60-day mortality (weighted HR 0.28) in CAPA patients.
2. 91.5% of CAPA patients received antifungals, predominantly azoles (90.7%), reflecting current practice patterns.
3. Immunosuppressive therapy doubled mortality risk (HR 2.08), while male sex showed protective effects (HR 0.61).
4. The study represents the largest CAPA treatment cohort to date (n=259) across five European centers.
Background: The Emerging Threat of CAPA
COVID-19-associated pulmonary aspergillosis (CAPA) has emerged as a lethal complication affecting 5-35% of ICU-admitted COVID-19 patients, with mortality rates exceeding 50% in early reports. The pathogenesis involves SARS-CoV-2-induced epithelial damage creating portals for Aspergillus invasion, compounded by immune dysregulation from corticosteroids and cytokine storms. Despite its clinical significance, optimal management remains contentious due to limited evidence from small cohorts.
Study Design: Rigorous Multinational Collaboration
This retrospective cohort analyzed 259 probable/proven CAPA cases from French hospitals and five European ICUs (2020 onward). Researchers employed:
- Cox regression with inverse probability treatment weighting
- Propensity score adjustment for baseline characteristics
- European Confederation of Medical Mycology (ECMM)/ISHAM diagnostic criteria
Key exposures included azole (voriconazole/isavuconazole) or polyene (amphotericin B) therapy, while the primary endpoint was 60-day all-cause mortality.
Key Findings: Mortality Benefit Persists After Adjustment
The raw population analysis revealed:
- Antifungals reduced mortality by 69% (HR 0.31, 95%CI:0.17-0.59)
- Immunosuppression increased mortality risk 2.08-fold
- Remdesivir showed unexpected mortality association (HR 1.96)
After propensity weighting, the mortality benefit held strong (HR 0.28, 95%CI:0.13-0.58), with number needed to treat estimated at 4. Subgroup analyses suggested consistent effects across azoles and polyenes, though sample sizes limited direct comparisons.
Expert Commentary: Urgent Implications for ICU Practice
Dr. Marcio Nucci (University of São Paulo), uninvolved in the study, noted: ‘These findings should settle the debate about CAPA treatment necessity. The signal is clear – delaying antifungals in probable CAPA risks avoidable deaths, especially in immunocompromised hosts.’ However, he cautioned about residual confounding from unmeasured variables like fungal burden.
Conclusion: A Call for Protocolized Screening
This study provides the strongest evidence to date supporting early antifungal therapy for CAPA, with particular urgency in immunocompromised patients. Future research should address:
- Optimal diagnostic algorithms combining galactomannan and PCR
- Comparative effectiveness of azoles vs. newer antifungals
- Biomarkers to identify treatment responders
For now, the data mandate heightened CAPA vigilance in COVID-19 ICUs worldwide.
Funding and Registration
Supported by the French Ministry of Health. No clinical trial registration (observational study).
References
1. Koehler P, et al. Lancet Infect Dis. 2021;21(6):e149-e162.
2. ECMM/ISHAM guidelines. Lancet Infect Dis. 2021;21(6):e149-e162.
3. Original study: Chest. 2026; PMID: 42002219.
