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Prevalence of CYP 3A5 Genomic Variances and Their Impact on Tacrolimus Dosing Requirements among Kidney Transplant Recipients in Eastern North Carolina
Author(s) -
Maldonado Angela Q.,
Asempa Tomefa,
Hudson Suzanne,
Rebellato Lorita M.
Publication year - 2017
Publication title -
pharmacotherapy: the journal of human pharmacology and drug therapy
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.227
H-Index - 109
eISSN - 1875-9114
pISSN - 0277-0008
DOI - 10.1002/phar.1970
Subject(s) - tacrolimus , dosing , cohort , immunosuppression , medicine , biology , transplantation
To assess the prevalence of CYP 3A5 genomic variances and their impact on tacrolimus (TAC) dosing requirements among kidney transplant recipients in eastern North Carolina, we conducted a single‐center retrospective cohort study at a large tertiary care medical center. A total of 162 adults who received a kidney transplant between March 1, 2013, and February 28, 2015, and received oral TAC as part of their maintenance immunosuppression were enrolled. Of these patients, 85 patients expressed a genotype with a CYP 3A5*1 variant ( C YP 3A5*1 group), and 77 patients expressed genotypes with other CYP 3A5 variants (nonexpressor group). All patients were followed for 1 year posttransplantation. The primary end point was the TAC total daily dose ( TDD ) required to achieve the first therapeutic trough level based on the presence or absence of the CYP 3A5*1 variant. The prevalence of different CYP 3A5 variants across race/ethnicities in the study cohort was determined by CYP 3A5 genotyping for each patient. The C YP 3A5*1 and nonexpressor groups did not differ significantly with respect to sex, mean age, or mean weight. The CYP 3A5*1 group was largely African American (93%, p≤0.0005) compared with other race/ethnicities. Among the CYP 3A5*1 expressors compared with nonexpressors, the mean TAC TDD in milligrams at the first therapeutic TAC level was significantly higher (12 vs 8 mg/day, p≤0.001). Similarly, the mean TAC TDD in milligrams/kilogram was 50% greater among CYP 3A5*1 expressors (0.15 vs 0.1 mg/kg/day, p≤0.0005). The predominant genotypic variants were CYP 3A5*3/*3 (33%), CYP 3A5*1/*3 (20%), and CYP 3A5*1/*1 (19%). This study illustrates the prevalence of the CYP 3A5*1 variant among African‐American kidney transplant recipients and the effect of this gene expression on the TAC TDD . Patients with the CYP 3A5*1 variant require higher TAC doses, on average, to achieve desirable drug levels. In addition, this study provides transplant clinicians with insight and support to dose TAC more aggressively in African‐American kidney transplant recipients who may be at higher risk for both toxicities as well as poor clinical outcomes related to inadequate immunosuppression.