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首页> 外文期刊>Biopharmaceutics and Drug Disposition >Estimation of absorption rate of alpha-human atrial natriuretic peptide from the plasma profile and diuretic effect after intranasal administration to rats.
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Estimation of absorption rate of alpha-human atrial natriuretic peptide from the plasma profile and diuretic effect after intranasal administration to rats.

机译:从大鼠鼻内给药后的血浆分布和利尿作用估计α-人心钠素的吸收率。

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The absorption rate of alpha-human atrial natriuretic peptide (alpha-hANP) after intranasal (i.n.) administration to rats was estimated from the plasma profile and pharmacological effect (diuretic effect) using a pharmacokinetic (PK) model and a PK-pharmacodynamic (PD) model involving data obtained after intravenous (i.v.) bolus injection. The plasma concentrations of alpha-hANP after i.v. administration at different doses were fitted to a two-compartment PK model with zero-order excretion and input of endogenous alpha-rat atrial natriuretic peptide (alpha-rANP) and two elimination processes represented by Michaelis-Menten and first-order kinetics. However, the saturable process was ignored at low doses. The plasma concentrations after low doses via the i.n. route could also be expressed by this model, but with first-order absorption, so that an absorption rate constant was calculated using a deconvolution method. In addition, the diuretic effect plotted against the i.v. dose was represented by the Hill equation and showed an anti-clockwise hysteresis loop versus the plasma concentration. These results suggest that the diuretic effect could be estimated by a PK-PD model having an 'effect' compartment or a homeostatic system. Such a PK-PD model accurately expressed the diuretic effect of alpha-hANP at all doses after i.v. and i.n. administrations. The resulting absorption rate constant calculated using the PK-PD model agreed closely with that obtained by the PK model alone. The absorption rate and simulated diuretic effect suggest that, for i.n. administration of alpha-hANP, a higher absorption rate constant causes a more potent diuretic effect (a dramatic effect over the early period), whereas greater bioavailability is associated with a better hypotensive effect (sustained effect).
机译:使用药代动力学(PK)模型和PK药效学(PD),根据血浆分布和药理作用(利尿作用)估算大鼠鼻内(服)后α-人心钠素(α-hANP)的吸收率)模型,涉及在静脉(iv)快速推注后获得的数据。静脉注射后血浆中的α-hANP浓度。以不同剂量进行的给药适合于具有零级排泄和输入内源性α-大鼠心房利钠肽(alpha-rANP)的两室PK模型,以及以Michaelis-Menten和一级动力学为代表的两个消除过程。但是,在低剂量时可饱和过程被忽略了。通过i.n.低剂量后的血浆浓度该路径也可以用该模型表示,但是具有一阶吸收,因此使用解卷积方法计算吸收速率常数。另外,利尿作用相对于静脉输注。剂量由希尔方程表示,并显示出相对于血浆浓度的逆时针磁滞回线。这些结果表明,利尿作用可以通过具有“作用”区室或体内平衡系统的PK-PD模型来估计。这种PK-PD模型在静脉注射后的所有剂量下都能准确表达出α-hANP的利尿作用。和i.n.行政部门。使用PK-PD模型计算出的吸收率常数与仅通过PK模型获得的吸收率常数非常吻合。吸收率和模拟的利尿作用表明施用α-hANP时,较高的吸收速率常数会导致更强的利尿作用(在早期阶段产生显着作用),而更大的生物利用度与更好的降压作用(持续作用)相关。

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