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A Predictive Model to Identify Complicated Clostridiodes difficile Infection
by
Micic, Dejan
, Lee, Allen
, Rifkin, Samara
, Steiner, Calen A
, Shirley, Daniel
, Higgins, Peter D R
, Young, Vincent B
, Alexander Perry, D
, Berinstein, Jeffrey A
, Rao, Krishna
in
Colorectal surgery
/ Infections
/ Intensive care
/ Major
2023
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A Predictive Model to Identify Complicated Clostridiodes difficile Infection
by
Micic, Dejan
, Lee, Allen
, Rifkin, Samara
, Steiner, Calen A
, Shirley, Daniel
, Higgins, Peter D R
, Young, Vincent B
, Alexander Perry, D
, Berinstein, Jeffrey A
, Rao, Krishna
in
Colorectal surgery
/ Infections
/ Intensive care
/ Major
2023
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Do you wish to request the book?
A Predictive Model to Identify Complicated Clostridiodes difficile Infection
by
Micic, Dejan
, Lee, Allen
, Rifkin, Samara
, Steiner, Calen A
, Shirley, Daniel
, Higgins, Peter D R
, Young, Vincent B
, Alexander Perry, D
, Berinstein, Jeffrey A
, Rao, Krishna
in
Colorectal surgery
/ Infections
/ Intensive care
/ Major
2023
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A Predictive Model to Identify Complicated Clostridiodes difficile Infection
Journal Article
A Predictive Model to Identify Complicated Clostridiodes difficile Infection
2023
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Overview
Abstract
Background
Clostridioides difficile infection (CDI) is a leading cause of health care–associated infection and may result in organ dysfunction, colectomy, and death. Published risk scores to predict severe complications from CDI demonstrate poor performance upon external validation. We hypothesized that building and validating a model using geographically and temporally distinct cohorts would more accurately predict risk for complications from CDI.
Methods
We conducted a multicenter retrospective cohort study of adults diagnosed with CDI. After randomly partitioning the data into training and validation sets, we developed and compared 3 machine learning algorithms (lasso regression, random forest, stacked ensemble) with 10-fold cross-validation to predict disease-related complications (intensive care unit admission, colectomy, or death attributable to CDI) within 30 days of diagnosis. Model performance was assessed using the area under the receiver operating curve (AUC).
Results
A total of 3646 patients with CDI were included, of whom 217 (6%) had complications. All 3 models performed well (AUC, 0.88–0.89). Variables of importance were similar across models, including albumin, bicarbonate, change in creatinine, non-CDI-related intensive care unit admission, and concomitant non-CDI antibiotics. Sensitivity analyses indicated that model performance was robust even when varying derivation cohort inclusion and CDI testing approach. However, race was an important modifier, with models showing worse performance in non-White patients.
Conclusions
Using a large heterogeneous population of patients, we developed and validated a prediction model that estimates risk for complications from CDI with good accuracy. Future studies should aim to reduce the disparity in model accuracy between White and non-White patients and to improve performance overall.
Publisher
Oxford University Press
Subject
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