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首页> 外文期刊>British Journal of Clinical Pharmacology >The pharmacokinetics of pioglitazone in patients with impaired renal function.
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The pharmacokinetics of pioglitazone in patients with impaired renal function.

机译:吡格列酮在肾功能受损患者中的药代动力学。

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摘要

AIMS: To evaluate the effect of renal impairment on the pharmacokinetics and safety of pioglitazone and its metabolites M-III and M-IV with impaired renal function and normal renal function. METHODS: In a phase-I, open-label, parallel-group study, six healthy subjects with normal renal function (creatinine clearance> 80 ml min-1), nine patients with moderate renal impairment (creatinine clearance 30-60 ml min-1) and 12 patients with severe renal impairment (creatinine clearance < 30 ml min-1) received single and multiple oral doses of pioglitazone 45 mg. The serum pharmacokinetic profiles of pioglitazone and its metabolites M-III and M-IV were assessed for the first and last dose administered (day 1 and day 12, respectively). RESULTS: Pharmacokinetic data revealed no significant accumulation of pioglitazone or its metabolites M-III and M-IV in patients with renal impairment. There was no significant difference in the pharmacokinetic profile of pioglitazone in subjects with normal and with moderately impaired renal function. After single oral doses, mean area under the concentration-time curve (AUC) values were decreased in patients with severe renal impairment compared with healthy subjects with normal renal function for pioglitazone (13 476 vs 17 387, P = 0.371; -23%; confidence interval (CI) -57, 38), M-III metabolite (13 394 vs 15 071, P = 0.841; -11%; CI -74, 194) and M-IV metabolite (27 991 vs 49 856, P = 0.006; -44%; CI -62, -17). After repeated oral doses of pioglitazone, mean AUC values ( micro g.h l-1) were decreased in patients with severe renal impairment compared with healthy subjects with normal renal function for pioglitazone (8744 vs 14,565, P = 0.004; -40%; CI -57, -16), M-III (3991 vs 7,289, P = 0.0009; -45%; CI -60, -25) and M-IV (21 080 vs 25 706, P = 0.181; -18%; CI 39, 10). The tolerability and safety profile of pioglitazone was comparable between groups. CONCLUSIONS: Pioglitazone was well tolerated in patients with varying degrees of renal impairment. Although mean serum concentrations of pioglitazone and its metabolites are increased in patients with severe renal impairment, adjustment of starting and maintenance doses in these patients is probably unwarranted.
机译:目的:评估肾功能不全对吡格列酮及其代谢产物M-III和M-IV肾功能受损和正常肾功能的药代动力学和安全性的影响。方法:在一项I期,开放标签,平行组研究中,六名健康的肾功能正常受试者(肌酐清除率> 80 ml min-1),九名中度肾功能不全(肌酐清除率30-60 ml min- 1)和12位严重肾功能不全(肌酐清除率<30 ml min-1)的患者接受单次和多次口服吡格列酮45 mg治疗。评估吡格列酮及其代谢产物M-III和M-IV的首次和最后一次给药(分别为第1天和第12天)的血清药代动力学特征。结果:药代动力学数据显示,在肾功能不全的患者中,吡格列酮或其代谢产物M-III和M-IV没有明显积累。在肾功能正常和中度受损的受试者中,吡格列酮的药代动力学特征无显着差异。单次口服后,与吡格列酮肾功能正常的健康受试者相比,重度肾功能不全患者的浓度-时间曲线(AUC)值平均面积降低了(13 476 vs 17 387,P = 0.371; -23%;和置信区间(CI)-57,38),M-III代谢产物(13 394 vs 15071,P = 0.841; -11%; CI -74,194)和M-IV代谢产物(27 991 vs 49 856,P = 0.006; -44%; CI -62,-17)。反复口服吡格列酮后,严重肾功能不全患者的平均AUC值(micro gh l-1)与吡格列酮肾功能正常的健康受试者相比有所降低(8744 vs 14,565,P = 0.004; -40%; CI- 57,-16),M-III(3991 vs 7,289,P = 0.0009; -45%; CI -60,-25)和M-IV(21 080 vs 25706,P = 0.181; -18%; CI 39 ,10)。吡格列酮的耐受性和安全性在两组之间相当。结论:不同程度的肾功能不全患者对吡格列酮的耐受性良好。尽管在患有严重肾功能不全的患者中吡格列酮及其代谢产物的平均血清浓度增加,但这些患者中开始剂量和维持剂量的调整可能没有必要。

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