Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis

UCC-SMART Study Group; Steven H.J. Hageman; Richard A.J. Post; Frank L.J. Visseren; J. William McEvoy; J. Wouter Jukema; Yvo Smulders; Maarten van Smeden; Jannick A.N. Dorresteijn

doi:10.1093/EURJPC/ZWAE175.313

Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis

UCC-SMART Study Group, Steven H.J. Hageman (Corresponding author), Richard A.J. Post, Frank L.J. Visseren, J. William McEvoy, J. Wouter Jukema, Yvo Smulders, Maarten van Smeden, Jannick A.N. Dorresteijn

Statistics

Research output: Contribution to journal › Meeting Abstract › Academic

Abstract

Background: Cardiovascular disease (CVD) risk scores provide point estimates of individual risk without uncertainty quantification. The objective of the current study was to demonstrate the feasibility and clinical utility of calculating uncertainty surrounding individual CVD-risk predictions using Bayesian methods. Study Design and Setting: Individuals with established atherosclerotic CVD were included from the Utrecht Cardiovascular Cohort—Secondary Manifestations of ARTerial disease (UCC-SMART). In 8,355 individuals, followed for median of 8.2 years (IQR 4.2–12.5), a Bayesian Weibull model was derived to predict the 10-year risk of recurrent CVD events. Results: Model coefficients and individual predictions from the Bayesian model were very similar to that of a traditional (‘frequentist’) model but the Bayesian model also predicted 95% credible intervals (CIs) surrounding individual risk estimates. The median width of the individual 95%CrI was 5.3% (IQR 3.6–6.5) and 17% of the population had a 95%CrI width of 10% or greater. The uncertainty decreased with increasing sample size used for derivation of the model. Combining the Bayesian Weibull model with sampled hazard ratios based on trial reports may be used to estimate individual estimates of absolute risk reduction with uncertainty measures and the probability that a treatment option will result in a clinically relevant risk reduction. Conclusion: Estimating uncertainty surrounding individual CVD risk predictions using Bayesian methods is feasible. The uncertainty regarding individual risk predictions could have several applications in clinical practice, like the comparison of different treatment options or by calculating the probability of the individual risk being below a certain treatment threshold. However, as the individual uncertainty measures only reflect sampling error and no biases in risk prediction, physicians should be familiar with the interpretation before widespread clinical adaption.

Original language	English
Article number	zwae175.313
Pages (from-to)	i463
Number of pages	1
Journal	European Journal of Preventive Cardiology
Volume	31
Issue number	suppl. 1
DOIs	https://doi.org/10.1093/EURJPC/ZWAE175.313
Publication status	Published - Jun 2024
Event	ESC Preventive Cardiology 2024 - Athens, Greece Duration: 25 Apr 2024 → 27 Apr 2024

Bibliographical note

Publisher Copyright:
© 2024 The Author(s)

Keywords

Bayesian
Cardiovascular
CI
Credible interval
Risk prediction
Uncertainty

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1093/EURJPC/ZWAE175.313

Cite this

UCC-SMART Study Group, Hageman, S. H. J., Post, R. A. J., Visseren, F. L. J., McEvoy, J. W., Jukema, J. W., Smulders, Y., van Smeden, M., & Dorresteijn, J. A. N. (2024). Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis. European Journal of Preventive Cardiology, 31(suppl. 1), i463. Article zwae175.313. https://doi.org/10.1093/EURJPC/ZWAE175.313

@article{57991feb11bb450d80578ab30212deb1,

title = "Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis",

abstract = "Background: Cardiovascular disease (CVD) risk scores provide point estimates of individual risk without uncertainty quantification. The objective of the current study was to demonstrate the feasibility and clinical utility of calculating uncertainty surrounding individual CVD-risk predictions using Bayesian methods. Study Design and Setting: Individuals with established atherosclerotic CVD were included from the Utrecht Cardiovascular Cohort—Secondary Manifestations of ARTerial disease (UCC-SMART). In 8,355 individuals, followed for median of 8.2 years (IQR 4.2–12.5), a Bayesian Weibull model was derived to predict the 10-year risk of recurrent CVD events. Results: Model coefficients and individual predictions from the Bayesian model were very similar to that of a traditional ({\textquoteleft}frequentist{\textquoteright}) model but the Bayesian model also predicted 95% credible intervals (CIs) surrounding individual risk estimates. The median width of the individual 95%CrI was 5.3% (IQR 3.6–6.5) and 17% of the population had a 95%CrI width of 10% or greater. The uncertainty decreased with increasing sample size used for derivation of the model. Combining the Bayesian Weibull model with sampled hazard ratios based on trial reports may be used to estimate individual estimates of absolute risk reduction with uncertainty measures and the probability that a treatment option will result in a clinically relevant risk reduction. Conclusion: Estimating uncertainty surrounding individual CVD risk predictions using Bayesian methods is feasible. The uncertainty regarding individual risk predictions could have several applications in clinical practice, like the comparison of different treatment options or by calculating the probability of the individual risk being below a certain treatment threshold. However, as the individual uncertainty measures only reflect sampling error and no biases in risk prediction, physicians should be familiar with the interpretation before widespread clinical adaption.",

keywords = "Bayesian, Cardiovascular, CI, Credible interval, Risk prediction, Uncertainty",

author = "{UCC-SMART Study Group} and Hageman, {Steven H.J.} and Post, {Richard A.J.} and Visseren, {Frank L.J.} and McEvoy, {J. William} and Jukema, {J. Wouter} and Yvo Smulders and {van Smeden}, Maarten and Dorresteijn, {Jannick A.N.}",

note = "Publisher Copyright: {\textcopyright} 2024 The Author(s); ESC Preventive Cardiology 2024 ; Conference date: 25-04-2024 Through 27-04-2024",

year = "2024",

month = jun,

doi = "10.1093/EURJPC/ZWAE175.313",

language = "English",

volume = "31",

pages = "i463",

journal = "European Journal of Preventive Cardiology",

issn = "2047-4873",

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UCC-SMART Study Group, Hageman, SHJ, Post, RAJ, Visseren, FLJ, McEvoy, JW, Jukema, JW, Smulders, Y, van Smeden, M & Dorresteijn, JAN 2024, 'Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis', European Journal of Preventive Cardiology, vol. 31, no. suppl. 1, zwae175.313, pp. i463. https://doi.org/10.1093/EURJPC/ZWAE175.313

Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis. / UCC-SMART Study Group; Hageman, Steven H.J. (Corresponding author); Post, Richard A.J. et al.
In: European Journal of Preventive Cardiology, Vol. 31, No. suppl. 1, zwae175.313, 06.2024, p. i463.

Research output: Contribution to journal › Meeting Abstract › Academic

TY - JOUR

T1 - Estimating uncertainty when providing individual cardiovascular risk predictions

T2 - ESC Preventive Cardiology 2024

AU - UCC-SMART Study Group

AU - Hageman, Steven H.J.

AU - Post, Richard A.J.

AU - Visseren, Frank L.J.

AU - McEvoy, J. William

AU - Jukema, J. Wouter

AU - Smulders, Yvo

AU - van Smeden, Maarten

AU - Dorresteijn, Jannick A.N.

PY - 2024/6

Y1 - 2024/6

N2 - Background: Cardiovascular disease (CVD) risk scores provide point estimates of individual risk without uncertainty quantification. The objective of the current study was to demonstrate the feasibility and clinical utility of calculating uncertainty surrounding individual CVD-risk predictions using Bayesian methods. Study Design and Setting: Individuals with established atherosclerotic CVD were included from the Utrecht Cardiovascular Cohort—Secondary Manifestations of ARTerial disease (UCC-SMART). In 8,355 individuals, followed for median of 8.2 years (IQR 4.2–12.5), a Bayesian Weibull model was derived to predict the 10-year risk of recurrent CVD events. Results: Model coefficients and individual predictions from the Bayesian model were very similar to that of a traditional (‘frequentist’) model but the Bayesian model also predicted 95% credible intervals (CIs) surrounding individual risk estimates. The median width of the individual 95%CrI was 5.3% (IQR 3.6–6.5) and 17% of the population had a 95%CrI width of 10% or greater. The uncertainty decreased with increasing sample size used for derivation of the model. Combining the Bayesian Weibull model with sampled hazard ratios based on trial reports may be used to estimate individual estimates of absolute risk reduction with uncertainty measures and the probability that a treatment option will result in a clinically relevant risk reduction. Conclusion: Estimating uncertainty surrounding individual CVD risk predictions using Bayesian methods is feasible. The uncertainty regarding individual risk predictions could have several applications in clinical practice, like the comparison of different treatment options or by calculating the probability of the individual risk being below a certain treatment threshold. However, as the individual uncertainty measures only reflect sampling error and no biases in risk prediction, physicians should be familiar with the interpretation before widespread clinical adaption.

AB - Background: Cardiovascular disease (CVD) risk scores provide point estimates of individual risk without uncertainty quantification. The objective of the current study was to demonstrate the feasibility and clinical utility of calculating uncertainty surrounding individual CVD-risk predictions using Bayesian methods. Study Design and Setting: Individuals with established atherosclerotic CVD were included from the Utrecht Cardiovascular Cohort—Secondary Manifestations of ARTerial disease (UCC-SMART). In 8,355 individuals, followed for median of 8.2 years (IQR 4.2–12.5), a Bayesian Weibull model was derived to predict the 10-year risk of recurrent CVD events. Results: Model coefficients and individual predictions from the Bayesian model were very similar to that of a traditional (‘frequentist’) model but the Bayesian model also predicted 95% credible intervals (CIs) surrounding individual risk estimates. The median width of the individual 95%CrI was 5.3% (IQR 3.6–6.5) and 17% of the population had a 95%CrI width of 10% or greater. The uncertainty decreased with increasing sample size used for derivation of the model. Combining the Bayesian Weibull model with sampled hazard ratios based on trial reports may be used to estimate individual estimates of absolute risk reduction with uncertainty measures and the probability that a treatment option will result in a clinically relevant risk reduction. Conclusion: Estimating uncertainty surrounding individual CVD risk predictions using Bayesian methods is feasible. The uncertainty regarding individual risk predictions could have several applications in clinical practice, like the comparison of different treatment options or by calculating the probability of the individual risk being below a certain treatment threshold. However, as the individual uncertainty measures only reflect sampling error and no biases in risk prediction, physicians should be familiar with the interpretation before widespread clinical adaption.

KW - Bayesian

KW - Cardiovascular

KW - CI

KW - Credible interval

KW - Risk prediction

KW - Uncertainty

U2 - 10.1093/EURJPC/ZWAE175.313

DO - 10.1093/EURJPC/ZWAE175.313

M3 - Meeting Abstract

SN - 2047-4873

VL - 31

SP - i463

JO - European Journal of Preventive Cardiology

JF - European Journal of Preventive Cardiology

IS - suppl. 1

M1 - zwae175.313

Y2 - 25 April 2024 through 27 April 2024

ER -

Estimating uncertainty when providing individual cardiovascular risk predictions: a Bayesian survival analysis

Abstract

Bibliographical note

Keywords

UN SDGs

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