MATE1 Deficiency Exacerbates Dofetilide-Induced Proarrhythmia.
Muhammad Erfan UddinEric D EisenmannYang LiKevin M HuangDominique A GarrisonZahra TalebiAlice A GibsonYan JinMahesh R NepalIngrid M BonillaQiang FuXinxin SunAlec MillarMikhail TarasovChristopher E JayXiaoming CuiHeidi J EinolfRyan M PelisSakima A SmithPrzemysław B RadwańskiDouglas H SweetMartin F FrommMartin F FrommCynthia A CarnesShuiying HuAlex SparreboomPublished in: International journal of molecular sciences (2022)
Dofetilide is a rapid delayed rectifier potassium current inhibitor widely used to prevent the recurrence of atrial fibrillation and flutter. The clinical use of this drug is associated with increases in QTc interval, which predispose patients to ventricular cardiac arrhythmias. The mechanisms involved in the disposition of dofetilide, including its movement in and out of cardiomyocytes, remain unknown. Using a xenobiotic transporter screen, we identified MATE1 ( SLC47A1 ) as a transporter of dofetilide and found that genetic knockout or pharmacological inhibition of MATE1 in mice was associated with enhanced retention of dofetilide in cardiomyocytes and increased QTc prolongation. The urinary excretion of dofetilide was also dependent on the MATE1 genotype, and we found that this transport mechanism provides a mechanistic basis for previously recorded drug-drug interactions of dofetilide with various contraindicated drugs, including bictegravir, cimetidine, ketoconazole, and verapamil. The translational significance of these observations was examined with a physiologically-based pharmacokinetic model that adequately predicted the drug-drug interaction liabilities in humans. These findings support the thesis that MATE1 serves a conserved cardioprotective role by restricting excessive cellular accumulation and warrant caution against the concurrent administration of potent MATE1 inhibitors and cardiotoxic substrates with a narrow therapeutic window.
Keyphrases
- drug induced
- atrial fibrillation
- end stage renal disease
- catheter ablation
- left ventricular
- heart failure
- high glucose
- chronic kidney disease
- adverse drug
- ejection fraction
- newly diagnosed
- type diabetes
- emergency department
- left atrial
- gene expression
- adipose tissue
- high throughput
- physical activity
- endothelial cells
- transcription factor
- peritoneal dialysis
- radiation therapy
- diabetic rats
- patient reported outcomes
- rectal cancer
- smoking cessation
- stress induced
- weight loss
- free survival
- wild type
- direct oral anticoagulants