What question did this study set out to answer?

To analyze mortality risk factors in MRSA bacteremia patients receiving pharmacist-led vancomycin dosing.

January 14, 2026Open Access

P-1345. Machine Learning-driven Insights into Mortality Risk Among MRSA Bacteremia Patients on Pharmacist-led Vancomycin Dosing

Key Points

To analyze mortality risk factors in MRSA bacteremia patients receiving pharmacist-led vancomycin dosing.
Conducted a cohort study at Queen Elizabeth Hospital focusing on MRSA bacteremia patients.
Utilized pharmacist-led dosing adjustments based on therapeutic drug monitoring.
Employed XGBoost machine learning for predictive modeling of mortality using baseline characteristics.
Identified 65 patients, with 20% dying within 28 days post-pharmacist assessment.
Noted significant predictors of mortality included albumin and lactate dehydrogenase among others.
Achieved 78.5% accuracy in predicting 28-day mortality using the model.

Abstract

Abstract Background Vancomycin dosing strategies guided by therapeutic drug monitoring (TDM) data are advocated in serious methicillin-resistant Staphylococcus aureus (MRSA) infections. Pharmacist-led vancomycin dosing was started in 2020 at the Queen Elizabeth Hospital (QEH), Hong Kong SAR, China. Doses were adjusted by either area under curve/minimal inhibitory concentration (AUC/MIC) -guided or trough-guided monitoring, depending on patient characteristics. This study analyzed patients with MRSA bacteremia and factors linked to mortality. It was approved by the Hospital Authority Central Institutional Review Board (CIRB-2025-019-1). Table 1. Baseline characteristics of patients with MRSA bacteremia required vancomycin therapeutic drug monitoring: at/before the first pharmacist assessment Methods We identified adults admitted to the medical department of QEH and had at least one pharmacist-led dosing review for MRSA bacteremia. Thirty-eight baseline characteristics were compared between patients who survived or died within 28 days of the first pharmacist assessment. From these variables we predicted mortality by selecting potential predictors via a hybrid approach, combining statistical tests (p 0. 1) with feature importance from XGBoost machine learning algorithm. Results From 2020 to November 2024, 65 patients were identified. Twenty-one (32. 3%) were female and 15 (23. 1%) required renal dialysis. Vancomycin MIC was less than 1 μg/mL in 96. 9% of the 65 first MRSA blood isolates. Dosing was reviewed at a median of 5 times (IQR 3–8). Thirteen (20%) died within 28 days after the first pharmacist assessment. Table 1 shows the details. Six variables (sex, white blood cell, neutrophil, platelet, albumin, lactate dehydrogenase, and blood gas pH) were selected (p 0. 1). A XGBoost model predicted 28-day mortality in five-fold cross-validation and yielded a training error of 6. 5% (93. 5% accuracy), a test error of 21. 5% (78. 5% accuracy) and an AUC of 0. 73. Platelet, albumin, and blood gas pH were the 3 most important features which contributed 46. 1%, 39. 7%, and 14. 1% to predications respectively. Cut-offs to predict mortality were 199 cells/10⁹/L (platelet), 19 g/L (albumin), and 7. 44 (blood gas pH). Conclusion Despite individualized vancomycin dosing, MRSA bacteremia still carries a high mortality risk. By modeling, platelet, albumin, and blood gas pH might be important predictors in this cohort. More studies with larger sample sizes are needed. Disclosures All Authors: No reported disclosures

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