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首页> 外文期刊>The Journal of Clinical Pharmacology: Official Journal of the American College of Clinical Pharmacology >Pharmacokinetics of M100240 and MDL 100,173, a Dual Angiotensin-Converting Enzyme/Neutral Endopeptidase Inhibitor, in Healthy Young and Elderly Volunteers.
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Pharmacokinetics of M100240 and MDL 100,173, a Dual Angiotensin-Converting Enzyme/Neutral Endopeptidase Inhibitor, in Healthy Young and Elderly Volunteers.

机译:M100240和MDL 100,173(一种双重血管紧张素转化酶/中性内肽酶抑制剂)在健康的年轻和老年人志愿者中的药代动力学。

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摘要

M100240 is an acetate thioester of MDL 100,173-a dual angiotensin-converting enzyme (ACE)eutral endopeptidase (NEP) inhibitor-in phase II development. The pharmacokinetics of M100240 and MDL 100,173 were compared in young and elderly subjects. Pharmacokinetic data were obtained from 12 young (ages 18-45 years, 10 male, 2 female) and 12 elderly (ages 65-85 years, 7 male, 5 female) healthy subjects in a parallel-group, open-label study. Following an overnight fast, subjects received a single 25-mg oral dose of M100240. Serial plasma concentrations of M100240 and MDL 100,173 were determined using a validated liquid chromatography/tandem mass spectrometry (LC/MS/MS) method, and pharmacokinetic parameters were calculated with noncompartmental methods. Single-dose treatment with M100240 was well tolerated in both groups of subjects, with no clinically significant changes in vital signs, ECG recordings, or laboratory safety parameters. M100240 was rapidly absorbed and converted to MDL 100,173, with M100240 concentrations no longer detectable at 3 to 4 hours postdose in both groups. The pharmacokinetics of the pharmacologically active MDL 100,173 were similar for both groups. Although maximum concentrations of M100240 were generally higher in elderly versus young subjects (C(max) 0.48 ng/mL vs. 0.17 ng/mL), systemic availability of M100240 was quite low and variable with plasma, and this apparent difference in parent drug exposure is unlikely to have important clinical implications. No age-related differences in the pharmacokinetic parameters of MDL 100,173 (C(max) 8.16 vs. 9.62 ng/mL, t(max) 1.25 vs. 1.5 h, AUC((0-last)) 81.6 vs. 72.2 ng*h/mL) were observed between young and elderly subjects, respectively. In conclusion, there are no age-related differences in the pharmacokinetics of MDL 100,173 between young and elderly subjects.
机译:M100240是MDL 100,173(一种双重血管紧张素转化酶(ACE)/中性内肽酶(NEP)抑制剂)处于II期开发的乙酸盐硫酯。比较了年轻和老年受试者的M100240和MDL 100,173的药代动力学。在平行组,开放标签研究中,从12位青年(18-45岁,男性10位,女性2位)和12位老年(65-85岁,7位男性,5位女性)健康受试者中获得了药代动力学数据。过夜禁食后,受试者接受25 mg的M100240单次口服剂量。使用验证的液相色谱/串联质谱法(LC / MS / MS)确定M100240和MDL 100,173的系列血浆浓度,并用非房室方法计算药代动力学参数。在两组受试者中,M100240的单剂量治疗均耐受良好,生命体征,ECG记录或实验室安全性参数无临床显着变化。 M100240被快速吸收并转化为MDL 100,173,两组均在给药后3至4小时不再检测到M100240浓度。两组的药理活性MDL 100,173的药代动力学相似。尽管老年人中M100240的最大浓度通常较高(C(最大)0.48 ng / mL对0.17 ng / mL),但是M100240的全身利用率非常低,并且随血浆而变化,并且母体药物暴露的明显差异不太可能具有重要的临床意义。 MDL 100,173的药代动力学参数无年龄相关差异(C(max)8.16 vs. 9.62 ng / mL,t(max)1.25 vs. 1.5 h,AUC((0-last))81.6 vs. 72.2 ng * h / mL)分别在年轻和老年受试者之间观察到。总之,在年轻和老年受试者之间,MDL 100,173的药代动力学没有与年龄相关的差异。

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