The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study

Kordo Saeed; Darius Cameron Wilson; Frank Bloos; Philipp Schuetz; Yuri van der Does; Olle Melander; Pierre Hausfater; Jacopo M Legramante; Yann-Erick Claessens; Deveendra Amin; Mari Rosenqvist; Graham White; Beat Mueller; Maarten Limper; Carlota Clemente Callejo; Antonella Brandi; Marc-Alexis Macchi; Nicholas Cortes; Alexander Kutz; Peter Patka; María Cecilia Yañez; Sergio Bernardini; Nathalie Beau; Matthew Dryden; Eric C M van Gorp; Marilena Minieri; Louisa Chan; Pleunie P M Rood; Juan Gonzalez Del Castillo

doi:10.1186/s13054-019-2329-5

The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study

Kordo Saeed^*, Darius Cameron Wilson, Frank Bloos, Philipp Schuetz, Yuri van der Does, Olle Melander, Pierre Hausfater, Jacopo M Legramante, Yann-Erick Claessens, Deveendra Amin, Mari Rosenqvist, Graham White, Beat Mueller, Maarten Limper, Carlota Clemente Callejo, Antonella Brandi, Marc-Alexis Macchi, Nicholas Cortes, Alexander Kutz, Peter PatkaMaría Cecilia Yañez, Sergio Bernardini, Nathalie Beau, Matthew Dryden, Eric C M van Gorp, Marilena Minieri, Louisa Chan, Pleunie P M Rood, Juan Gonzalez Del Castillo

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Background: There is a lack of validated tools to assess potential disease progression and hospitalisation decisions in patients presenting to the emergency department (ED) with a suspected infection. This study aimed to identify suitable blood biomarkers (MR-proADM, PCT, lactate and CRP) or clinical scores (SIRS, SOFA, qSOFA, NEWS and CRB-65) to fulfil this unmet clinical need. Methods: An observational derivation patient cohort validated by an independent secondary analysis across nine EDs. Logistic and Cox regression, area under the receiver operating characteristic (AUROC) and Kaplan-Meier curves were used to assess performance. Disease progression was identified using a composite endpoint of 28-day mortality, ICU admission and hospitalisation > 10 days. Results: One thousand one hundred seventy-five derivation and 896 validation patients were analysed with respective 28-day mortality rates of 7.1% and 5.0%, and hospitalisation rates of 77.9% and 76.2%. MR-proADM showed greatest accuracy in predicting 28-day mortality and hospitalisation requirement across both cohorts. Patient subgroups with high MR-proADM concentrations (≥ 1.54 nmol/L) and low biomarker (PCT < 0.25 ng/mL, lactate < 2.0 mmol/L or CRP < 67 mg/L) or clinical score (SOFA < 2 points, qSOFA < 2 points, NEWS < 4 points or CRB-65 < 2 points) values were characterised by a significantly longer length of hospitalisation (p < 0.001), rate of ICU admission (p < 0.001), elevated mortality risk (e.g. SOFA, qSOFA and NEWS HR [95%CI], 45.5 [10.0-207.6], 23.4 [11.1-49.3] and 32.6 [9.4-113.6], respectively) and a greater number of disease progression events (p < 0.001), compared to similar subgroups with low MR-proADM concentrations (< 1.54 nmol/L). Increased out-patient treatment across both cohorts could be facilitated using a derivation-derived MR-proADM cut-off of < 0.87 nmol/L (15.0% and 16.6%), with decreased readmission rates and no mortalities. Conclusions: In patients presenting to the ED with a suspected infection, the blood biomarker MR-proADM could most accurately identify the likelihood of further disease progression. Incorporation into an early sepsis management protocol may therefore aid rapid decision-making in order to either initiate, escalate or intensify early treatment strategies, or identify patients suitable for safe out-patient treatment.

Original language	English
Article number	40
Journal	Critical care (London, England)
Volume	23
Issue number	1
DOIs	https://doi.org/10.1186/s13054-019-2329-5
Publication status	Published - 8 Feb 2019

Keywords

Disease progression
Emergency department
MR-proADM
SOFA
Sepsis
qSOFA

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Saeed, K., Wilson, D. C., Bloos, F., Schuetz, P., van der Does, Y., Melander, O., Hausfater, P., Legramante, J. M., Claessens, Y.-E., Amin, D., Rosenqvist, M., White, G., Mueller, B., Limper, M., Callejo, C. C., Brandi, A., Macchi, M.-A., Cortes, N., Kutz, A., ... Del Castillo, J. G. (2019). The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study. Critical care (London, England), 23(1), Article 40. https://doi.org/10.1186/s13054-019-2329-5

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title = "The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study",

abstract = "Background: There is a lack of validated tools to assess potential disease progression and hospitalisation decisions in patients presenting to the emergency department (ED) with a suspected infection. This study aimed to identify suitable blood biomarkers (MR-proADM, PCT, lactate and CRP) or clinical scores (SIRS, SOFA, qSOFA, NEWS and CRB-65) to fulfil this unmet clinical need. Methods: An observational derivation patient cohort validated by an independent secondary analysis across nine EDs. Logistic and Cox regression, area under the receiver operating characteristic (AUROC) and Kaplan-Meier curves were used to assess performance. Disease progression was identified using a composite endpoint of 28-day mortality, ICU admission and hospitalisation > 10 days. Results: One thousand one hundred seventy-five derivation and 896 validation patients were analysed with respective 28-day mortality rates of 7.1% and 5.0%, and hospitalisation rates of 77.9% and 76.2%. MR-proADM showed greatest accuracy in predicting 28-day mortality and hospitalisation requirement across both cohorts. Patient subgroups with high MR-proADM concentrations (≥ 1.54 nmol/L) and low biomarker (PCT < 0.25 ng/mL, lactate < 2.0 mmol/L or CRP < 67 mg/L) or clinical score (SOFA < 2 points, qSOFA < 2 points, NEWS < 4 points or CRB-65 < 2 points) values were characterised by a significantly longer length of hospitalisation (p < 0.001), rate of ICU admission (p < 0.001), elevated mortality risk (e.g. SOFA, qSOFA and NEWS HR [95%CI], 45.5 [10.0-207.6], 23.4 [11.1-49.3] and 32.6 [9.4-113.6], respectively) and a greater number of disease progression events (p < 0.001), compared to similar subgroups with low MR-proADM concentrations (< 1.54 nmol/L). Increased out-patient treatment across both cohorts could be facilitated using a derivation-derived MR-proADM cut-off of < 0.87 nmol/L (15.0% and 16.6%), with decreased readmission rates and no mortalities. Conclusions: In patients presenting to the ED with a suspected infection, the blood biomarker MR-proADM could most accurately identify the likelihood of further disease progression. Incorporation into an early sepsis management protocol may therefore aid rapid decision-making in order to either initiate, escalate or intensify early treatment strategies, or identify patients suitable for safe out-patient treatment.",

keywords = "Disease progression, Emergency department, MR-proADM, SOFA, Sepsis, qSOFA",

author = "Kordo Saeed and Wilson, {Darius Cameron} and Frank Bloos and Philipp Schuetz and {van der Does}, Yuri and Olle Melander and Pierre Hausfater and Legramante, {Jacopo M} and Yann-Erick Claessens and Deveendra Amin and Mari Rosenqvist and Graham White and Beat Mueller and Maarten Limper and Callejo, {Carlota Clemente} and Antonella Brandi and Marc-Alexis Macchi and Nicholas Cortes and Alexander Kutz and Peter Patka and Ya{\~n}ez, {Mar{\'i}a Cecilia} and Sergio Bernardini and Nathalie Beau and Matthew Dryden and {van Gorp}, {Eric C M} and Marilena Minieri and Louisa Chan and Rood, {Pleunie P M} and {Del Castillo}, {Juan Gonzalez}",

note = "Publisher Copyright: {\textcopyright} 2019 The Author(s).",

year = "2019",

month = feb,

day = "8",

doi = "10.1186/s13054-019-2329-5",

language = "English",

volume = "23",

journal = "Critical care (London, England)",

issn = "1466-609X",

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Saeed, K, Wilson, DC, Bloos, F, Schuetz, P, van der Does, Y, Melander, O, Hausfater, P, Legramante, JM, Claessens, Y-E, Amin, D, Rosenqvist, M, White, G, Mueller, B, Limper, M, Callejo, CC, Brandi, A, Macchi, M-A, Cortes, N, Kutz, A, Patka, P, Yañez, MC, Bernardini, S, Beau, N, Dryden, M, van Gorp, ECM, Minieri, M, Chan, L, Rood, PPM & Del Castillo, JG 2019, 'The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study', Critical care (London, England), vol. 23, no. 1, 40. https://doi.org/10.1186/s13054-019-2329-5

The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study. / Saeed, Kordo; Wilson, Darius Cameron; Bloos, Frank et al.
In: Critical care (London, England), Vol. 23, No. 1, 40, 08.02.2019.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - The early identification of disease progression in patients with suspected infection presenting to the emergency department

T2 - a multi-centre derivation and validation study

AU - Saeed, Kordo

AU - Wilson, Darius Cameron

AU - Bloos, Frank

AU - Schuetz, Philipp

AU - van der Does, Yuri

AU - Melander, Olle

AU - Hausfater, Pierre

AU - Legramante, Jacopo M

AU - Claessens, Yann-Erick

AU - Amin, Deveendra

AU - Rosenqvist, Mari

AU - White, Graham

AU - Mueller, Beat

AU - Limper, Maarten

AU - Callejo, Carlota Clemente

AU - Brandi, Antonella

AU - Macchi, Marc-Alexis

AU - Cortes, Nicholas

AU - Kutz, Alexander

AU - Patka, Peter

AU - Yañez, María Cecilia

AU - Bernardini, Sergio

AU - Beau, Nathalie

AU - Dryden, Matthew

AU - van Gorp, Eric C M

AU - Minieri, Marilena

AU - Chan, Louisa

AU - Rood, Pleunie P M

AU - Del Castillo, Juan Gonzalez

PY - 2019/2/8

Y1 - 2019/2/8

N2 - Background: There is a lack of validated tools to assess potential disease progression and hospitalisation decisions in patients presenting to the emergency department (ED) with a suspected infection. This study aimed to identify suitable blood biomarkers (MR-proADM, PCT, lactate and CRP) or clinical scores (SIRS, SOFA, qSOFA, NEWS and CRB-65) to fulfil this unmet clinical need. Methods: An observational derivation patient cohort validated by an independent secondary analysis across nine EDs. Logistic and Cox regression, area under the receiver operating characteristic (AUROC) and Kaplan-Meier curves were used to assess performance. Disease progression was identified using a composite endpoint of 28-day mortality, ICU admission and hospitalisation > 10 days. Results: One thousand one hundred seventy-five derivation and 896 validation patients were analysed with respective 28-day mortality rates of 7.1% and 5.0%, and hospitalisation rates of 77.9% and 76.2%. MR-proADM showed greatest accuracy in predicting 28-day mortality and hospitalisation requirement across both cohorts. Patient subgroups with high MR-proADM concentrations (≥ 1.54 nmol/L) and low biomarker (PCT < 0.25 ng/mL, lactate < 2.0 mmol/L or CRP < 67 mg/L) or clinical score (SOFA < 2 points, qSOFA < 2 points, NEWS < 4 points or CRB-65 < 2 points) values were characterised by a significantly longer length of hospitalisation (p < 0.001), rate of ICU admission (p < 0.001), elevated mortality risk (e.g. SOFA, qSOFA and NEWS HR [95%CI], 45.5 [10.0-207.6], 23.4 [11.1-49.3] and 32.6 [9.4-113.6], respectively) and a greater number of disease progression events (p < 0.001), compared to similar subgroups with low MR-proADM concentrations (< 1.54 nmol/L). Increased out-patient treatment across both cohorts could be facilitated using a derivation-derived MR-proADM cut-off of < 0.87 nmol/L (15.0% and 16.6%), with decreased readmission rates and no mortalities. Conclusions: In patients presenting to the ED with a suspected infection, the blood biomarker MR-proADM could most accurately identify the likelihood of further disease progression. Incorporation into an early sepsis management protocol may therefore aid rapid decision-making in order to either initiate, escalate or intensify early treatment strategies, or identify patients suitable for safe out-patient treatment.

AB - Background: There is a lack of validated tools to assess potential disease progression and hospitalisation decisions in patients presenting to the emergency department (ED) with a suspected infection. This study aimed to identify suitable blood biomarkers (MR-proADM, PCT, lactate and CRP) or clinical scores (SIRS, SOFA, qSOFA, NEWS and CRB-65) to fulfil this unmet clinical need. Methods: An observational derivation patient cohort validated by an independent secondary analysis across nine EDs. Logistic and Cox regression, area under the receiver operating characteristic (AUROC) and Kaplan-Meier curves were used to assess performance. Disease progression was identified using a composite endpoint of 28-day mortality, ICU admission and hospitalisation > 10 days. Results: One thousand one hundred seventy-five derivation and 896 validation patients were analysed with respective 28-day mortality rates of 7.1% and 5.0%, and hospitalisation rates of 77.9% and 76.2%. MR-proADM showed greatest accuracy in predicting 28-day mortality and hospitalisation requirement across both cohorts. Patient subgroups with high MR-proADM concentrations (≥ 1.54 nmol/L) and low biomarker (PCT < 0.25 ng/mL, lactate < 2.0 mmol/L or CRP < 67 mg/L) or clinical score (SOFA < 2 points, qSOFA < 2 points, NEWS < 4 points or CRB-65 < 2 points) values were characterised by a significantly longer length of hospitalisation (p < 0.001), rate of ICU admission (p < 0.001), elevated mortality risk (e.g. SOFA, qSOFA and NEWS HR [95%CI], 45.5 [10.0-207.6], 23.4 [11.1-49.3] and 32.6 [9.4-113.6], respectively) and a greater number of disease progression events (p < 0.001), compared to similar subgroups with low MR-proADM concentrations (< 1.54 nmol/L). Increased out-patient treatment across both cohorts could be facilitated using a derivation-derived MR-proADM cut-off of < 0.87 nmol/L (15.0% and 16.6%), with decreased readmission rates and no mortalities. Conclusions: In patients presenting to the ED with a suspected infection, the blood biomarker MR-proADM could most accurately identify the likelihood of further disease progression. Incorporation into an early sepsis management protocol may therefore aid rapid decision-making in order to either initiate, escalate or intensify early treatment strategies, or identify patients suitable for safe out-patient treatment.

KW - Disease progression

KW - Emergency department

KW - MR-proADM

KW - SOFA

KW - Sepsis

KW - qSOFA

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U2 - 10.1186/s13054-019-2329-5

DO - 10.1186/s13054-019-2329-5

M3 - Article

C2 - 30736862

SN - 1466-609X

VL - 23

JO - Critical care (London, England)

JF - Critical care (London, England)

IS - 1

M1 - 40

ER -

The early identification of disease progression in patients with suspected infection presenting to the emergency department: a multi-centre derivation and validation study

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Keywords

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Correction to: The early identification of disease progression in patients with suspected infection presenting to the emergency department: A multi-centre derivation and validation study (Critical Care (2019) 23 (40) DOI: 10.1186/s13054-019-2329-5)

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