- Mehta, Rupal;
- Cai, Xuan;
- Lee, Jungwha;
- Xie, Dawei;
- Wang, Xue;
- Scialla, Julia;
- Anderson, Amanda H;
- Taliercio, Jon;
- Dobre, Mirela;
- Chen, Jing;
- Fischer, Michael;
- Leonard, Mary;
- Lash, James;
- Hsu, Chi-yuan;
- de Boer, Ian H;
- Feldman, Harold I;
- Wolf, Myles;
- Isakova, Tamara;
- Investigators, CRIC Study;
- Appel, Lawrence J;
- Go, Alan S;
- He, Jiang;
- Rao, Panduranga S;
- Rahman, Mahboob;
- Townsend, Raymond R
Rationale & objective
Studies using a single measurement of fibroblast growth factor 23 (FGF-23) suggest that elevated FGF-23 levels are associated with increased risk for requirement for kidney replacement therapy (KRT) in patients with chronic kidney disease. However, the data do not account for changes in FGF-23 levels as kidney disease progresses.Study design
Case-cohort study.Setting & participants
To evaluate the association between serial FGF-23 levels and risk for requiring KRT, our primary analysis included 1,597 individuals in the Chronic Renal Insufficiency Cohort Study who had up to 5 annual measurements of carboxy-terminal FGF-23. There were 1,135 randomly selected individuals, of whom 266 initiated KRT, and 462 individuals who initiated KRT outside the random subcohort.Exposure
Serial FGF-23 measurements and FGF-23 trajectory group membership.Outcomes
Incident KRT.Analytical approach
To handle time-dependent confounding, our primary analysis of time-updated FGF-23 levels used time-varying inverse probability weighting in a discrete time failure model. To compare our results with prior data, we used baseline and time-updated FGF-23 values in weighted Cox regression models. To examine the association of FGF-23 trajectory subgroups with risk for incident KRT, we used weighted Cox models with FGF-23 trajectory groups derived from group-based trajectory modeling as the exposure.Results
In our primary analysis, the HR for the KRT outcome per 1 SD increase in the mean of natural log-transformed (ln)FGF-23 in the past was 1.94 (95% CI, 1.51-2.49). In weighted Cox models using baseline and time-updated values, elevated FGF-23 level was associated with increased risk for incident KRT (HRs per 1 SD ln[FGF-23] of 1.18 [95% CI, 1.02-1.37] for baseline and 1.66 [95% CI, 1.49-1.86] for time-updated). Membership in the slowly and rapidly increasing FGF-23 trajectory groups was associated with ∼3- and ∼21-fold higher risk for incident KRT compared to membership in the stable FGF-23 trajectory group.Limitations
Residual confounding and lack of intact FGF-23 values.Conclusions
Increasing FGF-23 levels are independently associated with increased risk for incident KRT.