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首页> 外文期刊>Journal of Solution Chemistry >Second derivative spectrophotometric determination of the binding constant between codeine phosphate and bovine serum albumin
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Second derivative spectrophotometric determination of the binding constant between codeine phosphate and bovine serum albumin

机译:二阶导数分光光度法测定磷酸可待因与牛血清白蛋白之间的结合常数

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Second derivative spectrophotometry was applied to determine the binding constant (K) between codeine phosphate (COD) and bovine serum albumin (BSA) at simulated physiological conditions (37.00 °C and pH = 7.4). The second derivative spectra of COD in buffer solutions containing various amounts of BSA showed derivative isosbestic points. The residual background signals derived from incomplete suppression of BSA signals can be entirely eliminated in the second derivative spectra indicating that BSA has spectrophotometrically one kind of binding site for COD. The fractions of COD bound to BSA were calculated from the derivative intensity differences (ΔD values) of COD before and after the addition of BSA. Scatchard plot calculation suggested that the binding of COD to BSA can be explained by a partition-like non-specific binding model. The binding constant (K) was calculated from ΔD values according to the non-specific binding model by a nonlinear least-squares method. K values were almost constant for all of the COD concentrations studied with good reproducibility. The fractions predicted by the K values were in good agreement with the observed values. The results indicate the usefulness of the derivative method in drug-albumin binding studies without the need for prior separation procedures which may disturb the equilibrium states of the samples solutions.
机译:使用二阶导数分光光度法在模拟生理条件(37.00°C和pH = 7.4)下确定磷酸可待因(COD)与牛血清白蛋白(BSA)之间的结合常数(K)。在含有各种量的BSA的缓冲溶液中,COD的二阶导数光谱显示出了等渗点。在第二阶导数光谱中可以完全消除源自BSA信号不完全抑制的残留背景信号,这表明BSA具有分光光度法对COD的一种结合位点。从添加BSA之前和之后的COD的导数强度差(ΔD值)计算结合到BSA的COD的分数。斯卡查德图计算表明,COD与BSA的结合可以通过类似分区的非特异性结合模型来解释。根据非特异性结合模型,通过非线性最小二乘法从ΔD值算出结合常数(K)。对于所研究的所有COD浓度,K值几乎都是恒定的,并且具有良好的重现性。由K值预测的分数与观测值非常吻合。结果表明,导数法在药物-白蛋白结合研究中是有用的,无需事先进行可能会干扰样品溶液平衡状态的分离程序。

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