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头孢曲松的血浆蛋白结合率。

Plasma protein binding of ceftriaxone.

作者信息

Popick A C, Crouthamel W G, Bekersky I

机构信息

Department of Drug Metabolism, Hoffman-La Roche Inc., Nutley, NJ 07110.

出版信息

Xenobiotica. 1987 Oct;17(10):1139-45. doi: 10.3109/00498258709167406.

Abstract
  1. The plasma protein binding characteristics of ceftriaxone, a new cephalosporin antibiotic, were determined in human, baboon, rabbit, dog and rat plasma. 2. The protein binding of ceftriaxone was similar and concentration-dependent in human, baboon, rabbit and rat plasma, being highly bound (90-95%) at low concentrations (less than 100 micrograms/ml) but considerably less bound (approx. 60%) at high concentrations (greater than 400 micrograms/ml). Binding in dog plasma was also concentration-dependent but much lower (approx. 25%) at lower concentrations (30 micrograms/ml) and virtually unbound (2%) at high concentrations (1 mg/ml) over a similar concentration range. 3. Binding of ceftriaxone to human plasma involved two sites: a high affinity-low capacity (saturable) site and a low affinity-high capacity site. Binding to dog plasma apparently was at a single, high affinity-low capacity site. 4. The pharmacokinetics of ceftriaxone in an animal species with binding characteristics similar to man (baboon), appear to be non-linear when based on total drug concentration and linear when based on the free drug concentration. In the dog, pharmacokinetic parameters did not change appreciably if calculated from total or free drug concentrations, due to the low protein binding.
摘要
  1. 在人、狒狒、兔、狗和大鼠血浆中测定了新型头孢菌素抗生素头孢曲松的血浆蛋白结合特性。2. 头孢曲松在人、狒狒、兔和大鼠血浆中的蛋白结合情况相似且呈浓度依赖性,在低浓度(低于100微克/毫升)时高度结合(90 - 95%),但在高浓度(高于400微克/毫升)时结合程度显著降低(约60%)。在狗血浆中的结合也呈浓度依赖性,但在较低浓度(30微克/毫升)时低得多(约25%),在类似浓度范围内高浓度(1毫克/毫升)时几乎不结合(2%)。3. 头孢曲松与人血浆的结合涉及两个位点:一个高亲和力 - 低容量(可饱和)位点和一个低亲和力 - 高容量位点。与狗血浆的结合显然位于单一的高亲和力 - 低容量位点。4. 在具有与人相似结合特性的动物物种(狒狒)中,基于总药物浓度时头孢曲松的药代动力学似乎是非线性的,而基于游离药物浓度时是线性的。在狗中,由于蛋白结合率低,从总药物浓度或游离药物浓度计算时药代动力学参数没有明显变化。

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