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首页> 外文期刊>Biopharmaceutics and Drug Disposition >Estimation of serum protein binding of compounds metabolized in serum using matrix inhibition.
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Estimation of serum protein binding of compounds metabolized in serum using matrix inhibition.

机译:使用基质抑制评估血清中代谢的化合物的血清蛋白结合。

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It is difficult to evaluate the serum protein binding of compounds that are metabolized in rat serum, even when using ultrafiltration. Protein binding was estimated using matrix inhibition, a method that uses the change in metabolic velocity achieved by changing the free fraction of a compound in the incubation mixture by diluting the serum with phosphate buffered saline. The T(1/2) of phenyl nicotinate, benzyl nicotinate, octyl nicotinate, hexyl nicotinate, butyl nicotinate and [(3)H] compound A were 0.165, 0.780, 2.62, 3.94, 5.22 and 135 min, respectively, with protein binding values of 82.1%, 91.6%, 98.8%, 98.5%, 85.5% and 96.9%. The protein binding value of compound A estimated by ultrafiltration was 93.4%, indicating that the two methods give similar values. The matrix inhibition method is thus applicable for the evaluation of compounds metabolized in serum, and provides a simple, useful method to determine protein binding. Copyright (c) 2008 John Wiley & Sons, Ltd.
机译:即使使用超滤,也很难评估在大鼠血清中代谢的化合物的血清蛋白结合。使用基质抑制法评估蛋白质结合,该方法利用代谢速度的变化,该变化是通过用磷酸盐缓冲液稀释血清来改变孵育混合物中化合物的游离分数而实现的。烟酸苯酯,烟酸苄酯,烟酸辛酯,烟酸己酯,烟酸丁酯和[(3)H]化合物A的T(1/2)分别为0.165、0.780、2.62、3.94、5.22和135分钟,并具有蛋白质结合值分别为82.1%,91.6%,98.8%,98.5%,85.5%和96.9%。通过超滤估计的化合物A的蛋白质结合值为93.4%,表明两种方法给出的值相似。因此,基质抑制方法可用于评估血清中代谢的化合物,并提供一种简单,有用的方法来确定蛋白质结合。版权所有(c)2008 John Wiley&Sons,Ltd.

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