- © 2013 Marshfield Clinic
Does CALU SNP rs1043550 Contribute Variability to Therapeutic Warfarin Dosing Requirements?
- Ingrid Glurich, PhD*⇑,
- Richard L. Berg, MS† and
- James K. Burmester, PhD‡
- *Marshfield Clinic Research Foundation, Marshfield, WI USA
- †Biomedical Informatics Research Center, Marshfield Clinic Research Foundation, Marshfield, WI USA
- ‡Clinical Research Center; Marshfield Clinic Research Foundation, Marshfield, WI USA
- Corresponding Author: Ingrid Glurich, PhD; Marshfield Clinic Research Foundation ; 1000 North Oak Avenue; Marshfield, WI 54449; Tel: (715) 389-3072; Fax: (715) 389-5757; Email: glurichi{at}mcrf.mfldclin.edu
Abstract
Objectives Calumenin, a molecular chaperone, exerts a regulatory effect on the vitamin K-dependent γ-carboxylation redox cycle that inhibits transfer of the reduced vitamin K from VKORC1, the pharmacological target of warfarin, to the γ-carboxylase. Because of its polymorphic structure and central role in the warfarin metabolic pathway, a contributory role for calumenin to warfarin dose variability has been posited. The current study sought to validate modulation of therapeutic dosing requirements by a single nucleotide polymorphisms (SNP) occurring in the calumenin gene (CALU) reported in previous studies. The CALU SNP was further modeled to detect interaction with SNPs occurring in VKORC1, CYP2C9, and CYP4F2 genes and characterize any additional contribution to variability in therapeutic warfarin dose requirement.
Setting The study was undertaken in an established, well-characterized cohort of subjects treated with warfarin in the Anticoagulation Clinic of Marshfield Clinic in Marshfield, Wisconsin.
Methods Subjects (N=491) previously genotyped for SNPS known to contribute variability to therapeutic warfarin dose requirement were genotyped for CALU SNP rs1043550, using TaqMan assays. Contribution of CALU SNP rs1043550 was modeled relative to other genotypic and phenotypic characteristics including gender, diagnosis, age, body surface area, underlying indication for warfarin, comorbidities, and pharmacological exposures. Interaction between SNPs impacting on warfarin dose requirements and calumenin SNPs was also modeled.
Results Small differences in warfarin dosing requirements detected among individuals encoding the mutant G allele in the calumenin SNP were not statistically or clinically significant relative to therapeutic warfarin dose requirement and did not independently contribute significantly to the warfarin dosing model. Interaction between calumenin and VKORC1 SNPs contributed only minor additional variability to that ascribed to the wild type VKORC1 genotype.
Conclusions The impact of the CALU SNP on warfarin dose variability was minor and did not contribute significantly to therapeutic warfarin dose requirement in our study cohort. While no contribution was noted for the SNP examined in the present study, further examination of interaction between genetic elements contributing major impact on therapeutic warfarin dose requirements and genes exhibiting a lesser contribution is warranted.
