4.3 Article

Validation of cardiogenic shock phenotypes in a mixed cardiac intensive care unit population

Journal

CATHETERIZATION AND CARDIOVASCULAR INTERVENTIONS
Volume 99, Issue 4, Pages 1006-1014

Publisher

WILEY
DOI: 10.1002/ccd.30103

Keywords

acute coronary syndromes; cardiac intensive care unit; cardiogenic shock; machine learning; phenotypes; shock

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In this study, researchers identified three distinct phenotypic clusters within CICU patients with CS using agnostic K means clustering, and found differences in in-hospital and 1-year mortality among these clusters, with the highest severity of illness in Cluster 3.
Background Proposed phenotypes have recently been identified in cardiogenic shock (CS) populations using unsupervised machine learning clustering methods. We sought to validate these phenotypes in a mixed cardiac intensive care unit (CICU) population of patients with CS. Methods We included Mayo Clinic CICU patients admitted from 2007 to 2018 with CS. Agnostic K means clustering was used to assign patients to three clusters based on admission values of estimated glomerular filtration rate, bicarbonate, alanine aminotransferase, lactate, platelets, and white blood cell count. In-hospital mortality and 1-year mortality were analyzed using logistic regression and Cox proportional-hazards models, respectively. Results We included 1498 CS patients with a mean age of 67.8 +/- 13.9 years, and 37.1% were females. The acute coronary syndrome was present in 57.3%, and cardiac arrest was present in 34.0%. Patients were assigned to clusters as follows: Cluster 1 (noncongested), 603 (40.2%); Cluster 2 (cardiorenal), 452 (30.2%); and Cluster 3 (hemometabolic), 443 (29.6%). Clinical, laboratory, and echocardiographic characteristics differed across clusters, with the greatest illness severity in Cluster 3. Cluster assignment was associated with in-hospital mortality across subgroups. In-hospital mortality was higher in Cluster 3 (adjusted odds ratio [OR]: 2.6 vs. Cluster 1 and adjusted OR: 2.0 vs. Cluster 2, both p < 0.001). Adjusted 1-year mortality was incrementally higher in Cluster 3 versus Cluster 2 versus Cluster 1 (all p < 0.01). Conclusions We observed similar phenotypes in CICU patients with CS as previously reported, identifying a gradient in both in-hospital and 1-year mortality by cluster. Identifying these clinical phenotypes can improve mortality risk stratification for CS patients beyond standard measures.

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