Interactions between FGF23 and Genotype in Autosomal Dominant Polycystic Kidney Disease

Laura Grau; Berenice Gitomer; Bryan McNair; Myles Wolf; Peter Harris; Godela Brosnahan; Vicente Torres; Theodore Steinman; Alan Yu; Arlene Chapman; Michel Chonchol; Kristen L Nowak

doi:10.34067/KID.0001692020

Interactions between FGF23 and Genotype in Autosomal Dominant Polycystic Kidney Disease

Kidney360. 2020 Jul;1(7):648-656. doi: 10.34067/KID.0001692020. Epub 2020 Jul 30.

Authors

Laura Grau¹, Berenice Gitomer², Bryan McNair¹, Myles Wolf³, Peter Harris⁴, Godela Brosnahan^{1

2}, Vicente Torres⁴, Theodore Steinman⁵, Alan Yu⁶, Arlene Chapman⁷, Michel Chonchol^{1

2}, Kristen L Nowak^{1

2}

Affiliations

¹ Department of Biostatistics and Informatics, University of Colorado Anschutz Medical Campus, Aurora, Colorado.
² Division of Renal Diseases and Hypertension, University of Colorado Anschutz Medical Campus, Aurora, Colorado.
³ Division of Nephrology, Duke University, Durham, North Carolina.
⁴ Division of Nephrology & Hypertension, Mayo Clinic, Rochester, Minnesota.
⁵ Renal Division, Beth Israel Deaconess Medical Center, Boston, Massachusetts.
⁶ Division of Nephrology and Hypertension, University of Kansas Medical Center, Kansas City, Kansas.
⁷ Section of Nephrology, University of Chicago, Chicago, Illinois.

Abstract

Background: Higher serum intact fibroblast growth factor 23 (iFGF23) was associated with disease progression in participants with autosomal dominant polycystic kidney disease (ADPKD) in the HALT-PKD Studies. PKD mutation is also an important determinant of progression. We hypothesized that serum levels of iFGF23 and vitamin D metabolites (1,25-dihydroxyvitamin D [1,25(OH)₂D] and 25-hydroxyvitamin D [25[OH]D]) differ according to ADPKD mutation and differentially predict clinical end points according to genotype (significant interaction between genotype and mineral metabolites).

Methods: A total of 864 individuals with ADPKD who participated in the HALT-PKD Study A or B and had measurements of mineral metabolites (1,25[OH]₂D, 25[OH]D, iFGF23) were categorized by PKD mutation (PKD1 truncating, PKD1 nontruncating, PKD2, or no mutation detected [NMD]). The association of the interactions of genotype × iFGF23, genotype × 1,25(OH)2D, and genotype × 25(OH)D with (1) annualized change in eGFR; (2) mean annualized percentage change in height-corrected total kidney volume (Study A only); and (3) time to a composite of 50% reduction in eGFR, ESKD, or death were evaluated using linear regression and Cox proportional hazards regression.

Results: Median (interquartile range) iFGF23 differed (PKD1 truncating, 55.8 [40.7-76.8]; PKD1 nontruncating, 49.9 [37.7-71.0]; PKD2, 49.0 [33.8-70.5]; NMD, 50.3 [39.7-67.4] pg/ml; P=0.03) and mean±SD 1,25(OH)₂D differed (PKD1 truncating, 32.8±12.8; PKD1 nontruncating, 33.4±12.5; PKD2, 34.1±13.1; NMD, 38.0±14.6 pg/ml; P=0.02) according to PKD genotype. There was a significant interaction between iFGF23 and genotype (P=0.02) for the composite end point in fully adjusted models, but no significant interaction between 1,25(OH)₂D or 25(OH)D and genotype for clinical end points.

Conclusions: ADPKD genotype interacts significantly with FGF23 to influence clinical end points. Whereas the worst outcomes were in individuals with a PKD1-truncating or -nontruncating mutation and the highest iFGF23 tertile, risk of the composite end point differed according to iFGF23 the most in the PKD1-nontruncating and PKD2 groups.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Genotype
Humans
Kidney
Mutation
Polycystic Kidney, Autosomal Dominant* / genetics
TRPP Cation Channels / genetics

Substances

TRPP Cation Channels

Abstract

Publication types

MeSH terms

Substances

Grants and funding