The acute-phase reactant C-reactive protein (CRP) increases rapidly during an infection. We tested the hypothesis that chronic
low-level increases in CRP are associated with an increased risk of infectious disease.
We studied
9660 individuals from a prospective general population cohort, including
3592 in whom infectious disease developed,
and another 60 896 individuals from a
cross-sectional general population study, of whom 13 332 developed
infectious disease;
55% were women, and the mean age was 57 years.
Hospital diagnoses of infections in 1977–2010 were based on International Classification of Diseases–coded
discharge records from the national Danish Patient Registry. We
measured CRP concentrations and conducted genotyping
for 4 CRP polymorphisms that increase CRP.
Individuals with CRP >10 mg/L were excluded because of possible
ongoing infection
at the time of testing.
Individuals
with CRP >3 mg/L had 1.2 and 1.7 times increased risk of infectious
disease, in the prospective general population
cohort and the cross-sectional general
population study, respectively, compared with individuals with CRP <1
mg/L. In the
combined populations, individuals in the highest
CRP tertile (compared with the lowest) had an increased risk of
bacterial
diseases (hazard ratio 1.7, 95% CI 1.6–1.8), but
not viral, mycosis, and parasitic diseases. The increased risk was
mainly
carried by pneumonia, sepsis, and particularly
gram-negative infections. None of the genotype combinations examined
conferred
an increased risk of infectious disease.
Chronic
low-level CRP increases were associated with increased risk of bacterial
infections, gram-negative infections in
particular. Genotypes associated with increases
in CRP were not associated with increased risk of infection.
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