The pediatric sepsis biomarker risk model

INTRODUCTION: The intrinsic heterogeneity of clinical septic shock is a major challenge. For clinical trials, individual patient management, and quality improvement efforts, it is unclear which patients are least likely to survive and thus benefit from alternative treatment approaches. A robust risk...

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Autores principales: Wong, Hector R, Salisbury, Shelia, Xiao, Qiang, Cvijanovich, Natalie Z, Hall, Mark, Allen, Geoffrey L, Thomas, Neal J, Freishtat, Robert J, Anas, Nick, Meyer, Keith, Checchia, Paul A, Lin, Richard, Shanley, Thomas P, Bigham, Michael T, Sen, Anita, Nowak, Jeffrey, Quasney, Michael, Henricksen, Jared W, Chopra, Arun, Banschbach, Sharon, Beckman, Eileen, Harmon, Kelli, Lahni, Patrick, Lindsell, Christopher J
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3682273/
https://www.ncbi.nlm.nih.gov/pubmed/23025259
http://dx.doi.org/10.1186/cc11652
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author Wong, Hector R
Salisbury, Shelia
Xiao, Qiang
Cvijanovich, Natalie Z
Hall, Mark
Allen, Geoffrey L
Thomas, Neal J
Freishtat, Robert J
Anas, Nick
Meyer, Keith
Checchia, Paul A
Lin, Richard
Shanley, Thomas P
Bigham, Michael T
Sen, Anita
Nowak, Jeffrey
Quasney, Michael
Henricksen, Jared W
Chopra, Arun
Banschbach, Sharon
Beckman, Eileen
Harmon, Kelli
Lahni, Patrick
Lindsell, Christopher J
author_facet Wong, Hector R
Salisbury, Shelia
Xiao, Qiang
Cvijanovich, Natalie Z
Hall, Mark
Allen, Geoffrey L
Thomas, Neal J
Freishtat, Robert J
Anas, Nick
Meyer, Keith
Checchia, Paul A
Lin, Richard
Shanley, Thomas P
Bigham, Michael T
Sen, Anita
Nowak, Jeffrey
Quasney, Michael
Henricksen, Jared W
Chopra, Arun
Banschbach, Sharon
Beckman, Eileen
Harmon, Kelli
Lahni, Patrick
Lindsell, Christopher J
author_sort Wong, Hector R
collection PubMed
description INTRODUCTION: The intrinsic heterogeneity of clinical septic shock is a major challenge. For clinical trials, individual patient management, and quality improvement efforts, it is unclear which patients are least likely to survive and thus benefit from alternative treatment approaches. A robust risk stratification tool would greatly aid decision-making. The objective of our study was to derive and test a multi-biomarker-based risk model to predict outcome in pediatric septic shock. METHODS: Twelve candidate serum protein stratification biomarkers were identified from previous genome-wide expression profiling. To derive the risk stratification tool, biomarkers were measured in serum samples from 220 unselected children with septic shock, obtained during the first 24 hours of admission to the intensive care unit. Classification and Regression Tree (CART) analysis was used to generate a decision tree to predict 28-day all-cause mortality based on both biomarkers and clinical variables. The derived tree was subsequently tested in an independent cohort of 135 children with septic shock. RESULTS: The derived decision tree included five biomarkers. In the derivation cohort, sensitivity for mortality was 91% (95% CI 70 - 98), specificity was 86% (80 - 90), positive predictive value was 43% (29 - 58), and negative predictive value was 99% (95 - 100). When applied to the test cohort, sensitivity was 89% (64 - 98) and specificity was 64% (55 - 73). In an updated model including all 355 subjects in the combined derivation and test cohorts, sensitivity for mortality was 93% (79 - 98), specificity was 74% (69 - 79), positive predictive value was 32% (24 - 41), and negative predictive value was 99% (96 - 100). False positive subjects in the updated model had greater illness severity compared to the true negative subjects, as measured by persistence of organ failure, length of stay, and intensive care unit free days. CONCLUSIONS: The pediatric sepsis biomarker risk model (PERSEVERE; PEdiatRic SEpsis biomarkEr Risk modEl) reliably identifies children at risk of death and greater illness severity from pediatric septic shock. PERSEVERE has the potential to substantially enhance clinical decision making, to adjust for risk in clinical trials, and to serve as a septic shock-specific quality metric.
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spelling pubmed-36822732013-06-25 The pediatric sepsis biomarker risk model Wong, Hector R Salisbury, Shelia Xiao, Qiang Cvijanovich, Natalie Z Hall, Mark Allen, Geoffrey L Thomas, Neal J Freishtat, Robert J Anas, Nick Meyer, Keith Checchia, Paul A Lin, Richard Shanley, Thomas P Bigham, Michael T Sen, Anita Nowak, Jeffrey Quasney, Michael Henricksen, Jared W Chopra, Arun Banschbach, Sharon Beckman, Eileen Harmon, Kelli Lahni, Patrick Lindsell, Christopher J Crit Care Research INTRODUCTION: The intrinsic heterogeneity of clinical septic shock is a major challenge. For clinical trials, individual patient management, and quality improvement efforts, it is unclear which patients are least likely to survive and thus benefit from alternative treatment approaches. A robust risk stratification tool would greatly aid decision-making. The objective of our study was to derive and test a multi-biomarker-based risk model to predict outcome in pediatric septic shock. METHODS: Twelve candidate serum protein stratification biomarkers were identified from previous genome-wide expression profiling. To derive the risk stratification tool, biomarkers were measured in serum samples from 220 unselected children with septic shock, obtained during the first 24 hours of admission to the intensive care unit. Classification and Regression Tree (CART) analysis was used to generate a decision tree to predict 28-day all-cause mortality based on both biomarkers and clinical variables. The derived tree was subsequently tested in an independent cohort of 135 children with septic shock. RESULTS: The derived decision tree included five biomarkers. In the derivation cohort, sensitivity for mortality was 91% (95% CI 70 - 98), specificity was 86% (80 - 90), positive predictive value was 43% (29 - 58), and negative predictive value was 99% (95 - 100). When applied to the test cohort, sensitivity was 89% (64 - 98) and specificity was 64% (55 - 73). In an updated model including all 355 subjects in the combined derivation and test cohorts, sensitivity for mortality was 93% (79 - 98), specificity was 74% (69 - 79), positive predictive value was 32% (24 - 41), and negative predictive value was 99% (96 - 100). False positive subjects in the updated model had greater illness severity compared to the true negative subjects, as measured by persistence of organ failure, length of stay, and intensive care unit free days. CONCLUSIONS: The pediatric sepsis biomarker risk model (PERSEVERE; PEdiatRic SEpsis biomarkEr Risk modEl) reliably identifies children at risk of death and greater illness severity from pediatric septic shock. PERSEVERE has the potential to substantially enhance clinical decision making, to adjust for risk in clinical trials, and to serve as a septic shock-specific quality metric. BioMed Central 2012 2012-10-01 /pmc/articles/PMC3682273/ /pubmed/23025259 http://dx.doi.org/10.1186/cc11652 Text en Copyright ©2012 Wong et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Wong, Hector R
Salisbury, Shelia
Xiao, Qiang
Cvijanovich, Natalie Z
Hall, Mark
Allen, Geoffrey L
Thomas, Neal J
Freishtat, Robert J
Anas, Nick
Meyer, Keith
Checchia, Paul A
Lin, Richard
Shanley, Thomas P
Bigham, Michael T
Sen, Anita
Nowak, Jeffrey
Quasney, Michael
Henricksen, Jared W
Chopra, Arun
Banschbach, Sharon
Beckman, Eileen
Harmon, Kelli
Lahni, Patrick
Lindsell, Christopher J
The pediatric sepsis biomarker risk model
title The pediatric sepsis biomarker risk model
title_full The pediatric sepsis biomarker risk model
title_fullStr The pediatric sepsis biomarker risk model
title_full_unstemmed The pediatric sepsis biomarker risk model
title_short The pediatric sepsis biomarker risk model
title_sort pediatric sepsis biomarker risk model
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3682273/
https://www.ncbi.nlm.nih.gov/pubmed/23025259
http://dx.doi.org/10.1186/cc11652
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