Clinical risk factors and blood protein biomarkers of 10-year pneumonia risk

Clinical risk factors and blood protein biomarkers of 10-year pneumonia risk

Chronic inflammation may increase susceptibility to pneumonia. To explore associations between clinical comorbidities, serum protein immunoassays, and long-term pneumonia risk. Framingham Heart Study Offspring Cohort participants ≥65 years were linked to their Centers for Medicare Services claims da...

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Veröffentlicht in:PloS one 2024-07, Vol.19 (7), p.e0296139
Hauptverfasser: Lee, Ming-Ming, Zuo, Yi, Steiling, Katrina, Mizgerd, Joseph P, Kalesan, Bindu, Walkey, Allan J
Format: Artikel
Sprache:eng
Schlagworte:
Aged
Aged, 80 and over
Biology and Life Sciences
Biomarkers
Biomarkers - blood
Blood proteins
Blood Proteins - analysis
Body mass index
C-reactive protein
Cardiac arrhythmia
Chronic illnesses
Cohort Studies
Comorbidity
Congestive heart failure
Diabetes
Diabetes mellitus
Exercise
Female
Heart failure
Humans
Immunoassay
Immunoassays
Inflammation
Kidney diseases
Kinases
Lung diseases
Male
Matrix metalloproteinases
Medicaid
Medicare
Medicine and Health Sciences
Metalloproteinase
Missing data
Offspring
Pneumonia
Pneumonia - blood
Pneumonia - epidemiology
Proteins
Research and Analysis Methods
Risk Factors
Serum proteins
Statistical analysis
United States - epidemiology
Variables
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Zusammenfassung:Chronic inflammation may increase susceptibility to pneumonia. To explore associations between clinical comorbidities, serum protein immunoassays, and long-term pneumonia risk. Framingham Heart Study Offspring Cohort participants ≥65 years were linked to their Centers for Medicare Services claims data. Clinical data and 88 serum protein immunoassays were evaluated for associations with 10-year incident pneumonia risk using Fine-Gray models for competing risks of death and least absolute shrinkage and selection operators for covariate selection. We identified 1,370 participants with immunoassays and linkage to Medicare data. During 10 years of follow up, 428 (31%) participants had a pneumonia diagnosis. Chronic pulmonary disease [subdistribution hazard ratio (SHR) 1.87; 95% confidence interval (CI), 1.33-2.61], current smoking (SHR 1.79, CI 1.31-2.45), heart failure (SHR 1.74, CI 1.10-2.74), atrial fibrillation/flutter (SHR 1.43, CI 1.06-1.93), diabetes (SHR 1.36, CI 1.05-1.75), hospitalization within one year (SHR 1.34, CI 1.09-1.65), and age (SHR 1.06 per year, CI 1.04-1.08) were associated with pneumonia. Three baseline serum protein measurements were associated with pneumonia risk independent of measured clinical factors: growth differentiation factor 15 (SHR 1.32; CI 1.02-1.69), C-reactive protein (SHR 1.16, CI 1.06-1.27) and matrix metallopeptidase 8 (SHR 1.14, CI 1.01-1.30). Addition of C-reactive protein to the clinical model improved prediction (Akaike information criterion 4950 from 4960; C-statistic of 0.64 from 0.62). Clinical comorbidities and serum immunoassays were predictive of pneumonia risk. C-reactive protein, a routinely-available measure of inflammation, modestly improved pneumonia risk prediction over clinical factors. Our findings support the hypothesis that prior inflammation may increase the risk of pneumonia.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0296139