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Inflammation and elevated levels of fibroblast growth factor 23 are independent risk factors for death in chronic kidney disease.

Kidney international | 2017

Inflammation is a consequence of chronic kidney disease (CKD) and is associated with adverse outcomes in many clinical settings. Inflammation stimulates production of fibroblast growth factor 23 (FGF23), high levels of which are independently associated with mortality in CKD. Few large-scale prospective studies have examined inflammation and mortality in patients with CKD, and none tested the interrelationships among inflammation, FGF23, and risk of death. Therefore, we conducted a prospective investigation of 3875 participants in the Chronic Renal Insufficiency Cohort (CRIC) study with CKD stages 2 to 4 to test the associations of baseline plasma interleukin-6, high-sensitivity C-reactive protein, and FGF23 levels with all-cause mortality, censoring at the onset of end-stage renal disease. During a median follow-up of 6.9 years, 550 participants died (20.5/1000 person-years) prior to end-stage renal disease. In separate multivariable-adjusted analyses, higher levels of interleukin-6 (hazard ratio per one standard deviation increase of natural log-transformed levels) 1.35 (95% confidence interval, 1.25-1.46), C-reactive protein 1.28 (1.16-1.40), and FGF23 1.45 (1.32-1.60) were each independently associated with increased risk of death. With further adjustment for FGF23, the risks of death associated with interleukin-6 and C-reactive protein were minimally attenuated. Compared to participants in the lowest quartiles of inflammation and FGF23, the multivariable-adjusted hazard ratio of death among those in the highest quartiles of both biomarkers was 4.38 (2.65-7.23) for interleukin-6 and FGF23, and 5.54 (3.04-10.09) for C-reactive protein and FGF23. Thus, elevated levels of interleukin-6, C-reactive protein, and FGF23 are independent risk factors for mortality in CKD.

Pubmed ID: 28017325 RIS Download

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Associated grants

  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK061028
  • Agency: NCATS NIH HHS, United States
    Id: UL1 TR000433
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK060984
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK061021
  • Agency: NCATS NIH HHS, United States
    Id: UL1 TR001878
  • Agency: NIGMS NIH HHS, United States
    Id: P30 GM103337
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK060980
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK099930
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK060963
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK076116
  • Agency: NCRR NIH HHS, United States
    Id: UL1 RR024131
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK102438
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK061022
  • Agency: NCATS NIH HHS, United States
    Id: UL1 TR000003
  • Agency: NIDDK NIH HHS, United States
    Id: K23 DK095949
  • Agency: NCATS NIH HHS, United States
    Id: UL1 TR000439
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK081374
  • Agency: NCATS NIH HHS, United States
    Id: UL1 TR000424
  • Agency: NCRR NIH HHS, United States
    Id: M01 RR016500
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK060902
  • Agency: NIDDK NIH HHS, United States
    Id: K24 DK093723
  • Agency: NIDDK NIH HHS, United States
    Id: U01 DK060990
  • Agency: NHLBI NIH HHS, United States
    Id: R01 HL128714
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK073665
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK110087
  • Agency: NIDDK NIH HHS, United States
    Id: R01 DK080033
  • Agency: NCRR NIH HHS, United States
    Id: UL1 RR029879

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