Participant selection algorithm.

Participant selection algorithm.

<div><p>Background</p><p>C-reactive protein (CRP) is a biomarker of inflammation used in diagnosis of inflammatory diseases and to guide treatment decisions. Variation in within-individual measured CRP may affect its clinical utility but estimates of within-individual variati...

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Bibliographic Details
Main Author: Alex Gough (16734033) (author)
Other Authors: Alice Sitch (396379) (author), Tom Marshall (154542) (author)
Published: 2025
Subjects:
Biochemistry
Biotechnology
Evolutionary Biology
Immunology
Cancer
Mental Health
Infectious Diseases
severe disease status
guide treatment decisions
comorbidity covariates extracted
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retrospective cohort study
patient median crp
median reported cv
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performed using data
individual measured variation
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previously reported
world data
limited data
crp data
world nature
whole population
variation increases
short half
reactive protein
primary care
previous studies
largest study
large number
inflammatory diseases
inflammation used
individual variation
inclusion criterion
important implications
dexter tool
database using
cv increased
clinical utility
clinical decision
approximately five
acute illness
606 ).
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Summary:<div><p>Background</p><p>C-reactive protein (CRP) is a biomarker of inflammation used in diagnosis of inflammatory diseases and to guide treatment decisions. Variation in within-individual measured CRP may affect its clinical utility but estimates of within-individual variation are based on limited data and so may not be accurate.</p><p>Methods</p><p>A retrospective cohort study was performed using data on CRP results and sociodemographic, lifestyle and comorbidity covariates extracted from the IQVIA Medical Research Database (IMRD) database using the DEXTER tool. A minimum of four measurements for each individual was the only inclusion criterion. CRP data were log-transformed for analysis. Within-individual measured variation was calculated as a coefficient of variation (CV) using a linear regression random effects model for the whole population and various subgroups.</p><p>Results</p><p>472,811 participants were included in this study, making it the largest study of variation of CRP to date by a factor of approximately five. The overall coefficient of variation for CRP was 1.604 (95% CI 1.602 to 1.606). This is much higher than the median reported CV for CRP of previous studies which was 0.41. CV increased with patient median.</p><p>Strengths and limitations</p><p>The large number of participants and the real-world nature of the results are important strengths of this study. Weaknesses included the problem of accounting for confounding by indication, and the short half-life of CRP making it hard to distinguish between acute illness and physiological variation.</p><p>Conclusions</p><p>Estimated within-individual variation in this analysis of real-world data is very high and is higher than previously reported. Variation increases with patient median CRP, that is with more severe disease status. This has important implications for the diagnosis, monitoring and clinical decision-making for inflammatory disease.</p></div>

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