What question did this study set out to answer?

Identify early clinical and laboratory markers that predict poor outcomes in children with sepsis-induced ARDS in a lower-middle-income country.

March 26, 2026

1389: Predictors of Poor Outcomes in Pediatric Sepsis-Induced Ards: Prospective Cohort Study From an Lmic

Key Points

Identify early clinical and laboratory markers that predict poor outcomes in children with sepsis-induced ARDS in a lower-middle-income country.
Conducted a 3-year prospective cohort study in a pediatric ICU.
Enrolled children aged 1 month to 18 years with sepsis and monitored for ARDS and mortality.
Recorded demographic data, severity scores, and laboratory parameters.
Used logistic regression to find independent predictors of ARDS and mortality.
44.2% of septic patients developed ARDS within 96 hours; overall mortality was 23.4%.
Non-survivors had higher VIS scores (0.84) compared to survivors (0.28).
Lactate levels were significantly higher in non-survivors (5.11 mmol/L) than survivors (3.67 mmol/L).
On multivariate analysis, Day 1 lactate independently predicted ARDS development (OR 1.21).

Abstract

Introduction: Pediatric ARDS (pARDS), often triggered by sepsis, carries a high mortality burden, particularly in resource-limited settings. While 75% of pediatric ARDS cases are sepsis-related, most predictive data derive from high-income countries. We hypothesized that simple clinical and laboratory markers collected early during ICU admission could predict poor outcomes in children with sepsis-induced ARDS in a lower-middle-income country (LMIC) setting. Methods: This was a 3-year prospective cohort study (2021–2023) conducted in the PICU at Aga Khan University Hospital, Karachi, Pakistan. Children aged 1 month to 18 years with sepsis were enrolled and monitored for ARDS development and mortality. Demographic data, severity scores (PELOD-2, VIS), and laboratory parameters (platelet count, creatinine, lactate) were recorded. ARDS was diagnosed based on PALICC criteria. Logistic regression was used to identify independent predictors of ARDS development and mortality. Results: Out of 128 septic patients, 44.2% developed ARDS within 96 hours, and overall mortality was 23.4%. Non-survivors were more likely to be immunocompromised (30% vs. 13.3%, p=0.03). Significant predictors of mortality included higher VIS at 24 hours (0.84 vs. 0.28, p< 0.001), elevated PELOD-2 scores (≥4 in 21.4% of non-survivors vs. 8.6% survivors), thrombocytopenia (117 vs. 193×103/µL, p=0.044), elevated creatinine (1.70 vs. 0.87 mg/dL, p=0.015), and increased lactate levels (5.11 vs. 3.67 mmol/L, p=0.007). Higher FiO2 requirements were also observed in non-survivors (p=0.023). On multivariate analysis, only lactate on Day 1 independently predicted ARDS development (OR 1.21, p=0.018). Conclusions: In LMIC PICUs, simple early markers—especially lactate, platelet count, and VIS—can aid in identifying children at high risk for ARDS and mortality. These low-cost indicators can guide early escalation in care, improve triage, and help validate context-specific severity scoring tools in resource-constrained settings.

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1389: Predictors of Poor Outcomes in Pediatric Sepsis-Induced Ards: Prospective Cohort Study From an Lmic

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Abstract

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