Your search keyword '"Michael G. S. Shashaty"' showing total 2 results

1. Association of vancomycin plus piperacillin-tazobactam with early changes in creatinine versus cystatin C in critically ill adults: a prospective cohort study

Author

Todd A, Miano, Sean, Hennessy, Wei, Yang, Thomas G, Dunn, Ariel R, Weisman, Oluwatosin, Oniyide, Roseline S, Agyekum, Alexandra P, Turner, Caroline A G, Ittner, Brian J, Anderson, F Perry, Wilson, Raymond, Townsend, John P, Reilly, Heather M, Giannini, Christopher V, Cosgriff, Tiffanie K, Jones, Nuala J, Meyer, and Michael G S, Shashaty

Subjects

Adult, Critical Illness, Penicillanic Acid, Acute Kidney Injury, Anti-Bacterial Agents, Piperacillin, Tazobactam Drug Combination, Renal Dialysis, Vancomycin, Creatinine, Humans, Drug Therapy, Combination, Prospective Studies, Cystatin C, Cefepime, Biomarkers, Retrospective Studies

Abstract

Although dozens of studies have associated vancomycin + piperacillin-tazobactam with increased acute kidney injury (AKI) risk, it is unclear whether the association represents true injury or a pseudotoxicity characterized by isolated effects on creatinine secretion. We tested this hypothesis by contrasting changes in creatinine concentration after antibiotic initiation with changes in cystatin C concentration, a kidney biomarker unaffected by tubular secretion.We included patients enrolled in the Molecular Epidemiology of SepsiS in the ICU (MESSI) prospective cohort who were treated for ≥ 48 h with vancomycin + piperacillin-tazobactam or vancomycin + cefepime. Kidney function biomarkers [creatinine, cystatin C, and blood urea nitrogen (BUN)] were measured before antibiotic treatment and at day two after initiation. Creatinine-defined AKI and dialysis were examined through day-14, and mortality through day-30. Inverse probability of treatment weighting was used to adjust for confounding. Multiple imputation was used to impute missing baseline covariates.The study included 739 patients (vancomycin + piperacillin-tazobactam n = 297, vancomycin + cefepime n = 442), of whom 192 had cystatin C measurements. Vancomycin + piperacillin-tazobactam was associated with a higher percentage increase of creatinine at day-two 8.04% (95% CI 1.21, 15.34) and higher incidence of creatinine-defined AKI: rate ratio (RR) 1.34 (95% CI 1.01, 1.78). In contrast, vancomycin + piperacillin-tazobactam was not associated with change in alternative biomarkers: cystatin C: - 5.63% (95% CI - 18.19, 8.86); BUN: - 4.51% (95% CI - 12.83, 4.59); or clinical outcomes: dialysis: RR 0.63 (95% CI 0.31, 1.29); mortality: RR 1.05 (95%CI 0.79, 1.41).Vancomycin + piperacillin-tazobactam was associated with creatinine-defined AKI, but not changes in alternative kidney biomarkers, dialysis, or mortality, supporting the hypothesis that vancomycin + piperacillin-tazobactam effects on creatinine represent pseudotoxicity.

Published

2022

2. A Multibiomarker-Based Outcome Risk Stratification Model for Adult Septic Shock*

Author

Hector R. Wong, Christopher J. Lindsell, Ville Pettilä, Nuala J. Meyer, Simone A. Thair, Sari Karlsson, James A. Russell, Christopher D. Fjell, John H. Boyd, Esko Ruokonen, Michael G. S. Shashaty, Jason D. Christie, Kimberly W. Hart, Patrick Lahni, and Keith R. Walley

Subjects

Adult, Oncology, medicine.medical_specialty, Critical Care and Intensive Care Medicine, Risk Assessment, Sensitivity and Specificity, Internal medicine, medicine, Humans, Hospital Mortality, Intensive care medicine, APACHE, Aged, Adult patients, business.industry, Septic shock, Age Factors, Middle Aged, Decision Support Systems, Clinical, Prognosis, medicine.disease, Shock, Septic, Intensive Care Units, Chronic disease, ROC Curve, Multicenter study, Shock (circulatory), Chronic Disease, Risk stratification, Biomarker (medicine), medicine.symptom, DNA Probes, business, Risk assessment, Biomarkers

Abstract

Clinical trials in septic shock continue to fail due, in part, to inequitable and sometimes unknown distribution of baseline mortality risk between study arms. Investigators advocate that interventional trials in septic shock require effective outcome risk stratification. We derived and tested a multibiomarker-based approach to estimate mortality risk in adults with septic shock.Previous genome-wide expression studies identified 12 plasma proteins as candidates for biomarker-based risk stratification. The current analysis used banked plasma samples and clinical data from existing studies. Biomarkers were assayed in plasma samples obtained from 341 subjects with septic shock within 24 hours of admission to the ICU. Classification and regression tree analysis was used to generate a decision tree predicting 28-day mortality based on a combination of both biomarkers and clinical variables. The derived tree was first tested in an independent cohort of 331 subjects, then calibrated using all subjects (n = 672), and subsequently validated in another independent cohort (n = 209).Multiple ICUs in Canada, Finland, and the United States.Eight hundred eighty-one adults with septic shock or severe sepsis.None.The derived decision tree included five candidate biomarkers, admission lactate concentration, age, and chronic disease burden. In the derivation cohort, sensitivity for mortality was 94% (95% CI, 87-97), specificity was 56% (50-63), positive predictive value was 50% (43-57), and negative predictive value was 95% (89-98). Performance was comparable in the test cohort. The calibrated decision tree had the following test characteristics in the validation cohort: sensitivity 85% (76-92), specificity 60% (51-69), positive predictive value 61% (52-70), and negative predictive value 85% (75-91).We have derived, tested, calibrated, and validated a risk stratification tool and found that it reliably estimates the probability of mortality in adults with septic shock.

Published

2014