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美法仑在健康人类和大鼠体内的血浆蛋白结合呈浓度依赖性。

Melphalan concentration dependent plasma protein binding in healthy humans and rats.

作者信息

Greig N H, Sweeney D J, Rapoport S I

出版信息

Eur J Clin Pharmacol. 1987;32(2):179-85. doi: 10.1007/BF00542192.

Abstract

The binding of melphalan to plasma proteins from four healthy humans and from rats was measured by centrifugal ultrafiltration. Melphalan concentrations were determined by HPLC and by measuring 14C-melphalan activity. In whole blood, melphalan was distributed preferentially in plasma. However, a constant fraction, 37%, which was independent of the total melphalan concentration in whole blood, was present within the red blood cells. The binding of melphalan to plasma proteins from humans was less than that from rats. In both, however, the fraction bound was constant throughout the concentration range (0.1 to 9.0 microM) that is achieved during standard-dose melphalan therapy. Albumin was the primary binding protein. At concentrations equal to or in excess of 33 microM, which have been achieved during high-dose melphalan therapy, free plasma melphalan concentrations were no longer linearly related to total drug concentrations, and the plasma protein binding of melphalan in the human became concentration dependent. This occurred at concentrations of 70 microM in the rat. Scatchard analysis of the data indicated the presence of 2 groups of binding sites. Class I sites had 0.03 and 0.4 binding sites per albumin molecule in humans and rats, with respective association constants of 4.43 X 10(4) M-1 and 1.92 X 10(4) M-1. Class II sites had 5.18 and 2.60 binding sites per molecule, with respective association constants of 3.82 X 10(2) M-1 and 2.01 X 10(2) M-1.

摘要

通过离心超滤法测定了美法仑与四名健康人和大鼠血浆蛋白的结合情况。美法仑浓度通过高效液相色谱法(HPLC)以及测量¹⁴C - 美法仑活性来确定。在全血中,美法仑优先分布于血浆中。然而,红细胞内存在一个恒定比例(37%),该比例与全血中美法仑的总浓度无关。美法仑与人血浆蛋白的结合少于与大鼠血浆蛋白的结合。不过,在标准剂量美法仑治疗期间所达到的浓度范围(0.1至9.0微摩尔)内,两者的结合比例均保持恒定。白蛋白是主要的结合蛋白。在高剂量美法仑治疗期间可达到的浓度等于或超过33微摩尔时,游离血浆美法仑浓度与总药物浓度不再呈线性关系,并且人血浆中美法仑的蛋白结合变得具有浓度依赖性。在大鼠中,该情况发生在浓度为70微摩尔时。对数据进行Scatchard分析表明存在两组结合位点。在人和大鼠中,I类位点每个白蛋白分子分别有0.03和0.4个结合位点,各自的缔合常数分别为4.43×10⁴ M⁻¹和1.92×10⁴ M⁻¹。II类位点每个分子分别有5.18和2.60个结合位点,各自的缔合常数分别为3.82×10² M⁻¹和2.01×10² M⁻¹。

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