首页> 美国卫生研究院文献>Iranian Journal of Pharmaceutical Research : IJPR >Impact of UGT1A9 Polymorphism on Mycophenolic Acid Pharmacokinetic Parameters in Stable Renal Transplant Patients
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Impact of UGT1A9 Polymorphism on Mycophenolic Acid Pharmacokinetic Parameters in Stable Renal Transplant Patients

机译:UGT1A9基因多态性对稳定肾移植患者霉酚酸药代动力学参数的影响

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摘要

There are wide individual differences in pharmacokinetic parameters of mycophenolate mofetil (MMF) among transplanted patients. Some studies have shown that single nucleotide polymorphisms (SNPs) of the Uridine Diphosphate Glucuronosyl Transferase1A9 (UGT1A9) are responsible for these differences in early days after transplantation. Therefore it was decided to evaluate the influence of UGT polymorphism on MMF pharmacokinetics among stable Iranian transplant patients. This was a cross sectional study from March 2008 through December 2008 in Imam Khomeini Hospital affiliated to the Tehran University of Medical Sciences in Iran. Blood samples were taken from 40 de novo stable Iranian renal transplant patients taking 2 g MMF daily with SrCr≤1.4 mg/dL with at least 3 months history of transplantation. Appropriate PCR and HPLC methods were used for the determination of SNPs and their impact on MPA pharmacokinetics. T-275A polymorphism occurred in 15% of patients, UGT1A9*3 occurred in 2.5% of patients. Carriers of T-275A polymorphism had significant lower MPA AUC 0-12 in comparison with non-carriers or wild type (73.3±17.8 g/h/mL vs. 110.8±31.1 μg/h/mL, p = 0.006). There was no significant difference in AUC 6-12 between the two groups although carriers of T-275A SNP had lower MPA AUC 6-12 (22.4±4.5 μg/h/mL vs. 26.8±10.2 μg/h/mL, p = 0.24). Cmax was lower in the carriers of (20.2±9.0 μg/mL vs. 37.2±12.5 μg/mL, p=0.004). There was no significant difference in C0 between two groups. (3.0±1.2 μg/mL vs. 3.9±1.6 μg/mL, p = 0.1). This study in Iranian stable transplanted patients shows that carriers of T-275A polymorphism had significantly lower MPA exposure compared to non-carriers.
机译:在移植患者中,霉酚酸酯(MMF)的药代动力学参数存在很大的个体差异。一些研究表明,尿苷二磷酸葡萄糖醛酸糖基转移酶1A9(UGT1A9)的单核苷酸多态性(SNPs)导致了移植后早期的这些差异。因此,决定评估UGT多态性对稳定的伊朗移植患者中MMF药代动力学的影响。这是从2008年3月至2008年12月在伊朗德黑兰医学大学附属的伊玛目霍梅尼医院进行的横断面研究。血液样本采自40名从头开始接受稳定研究的伊朗肾脏移植患者,他们每天服用2 g MMF,SrCr≤1.4mg / dL,并且至少有3个月的移植史。适当的PCR和HPLC方法用于测定SNP及其对MPA药代动力学的影响。 T-275A多态性发生在15%的患者中,UGT1A9 * 3发生在2.5%的患者中。与非载体或野生型相比,T-275A多态性载体的MPA AUC 0-12明显更低(73.3±17.8 g / h / mL与110.8±31.1μg/ h / mL,p = 0.006)。尽管T-275A SNP携带者的MPA AUC 6-12较低(22.4±4.5μg/ h / mL对比26.8±10.2μg/ h / mL,p = 2),但两组之间的AUC 6-12差异无统计学意义。 0.24)。载体中的Cmax较低(20.2±9.0μg/ mL对37.2±12.5μg/ mL,p = 0.004)。两组之间的C0无明显差异。 (3.0±1.2μg/ mL与3.9±1.6μg/ mL,p = 0.1)。这项针对伊朗稳定移植患者的研究表明,与非携带者相比,T-275A多态性携带者的MPA暴露显着降低。

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