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首页> 外文期刊>Pharmaceutical research >Accurate potentiometric determination of lipid membrane-water partition coefficients and apparent dissociation constants of ionizable drugs: electrostatic corrections.
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Accurate potentiometric determination of lipid membrane-water partition coefficients and apparent dissociation constants of ionizable drugs: electrostatic corrections.

机译:电位计准确测定脂质膜-水分配系数和可电离药物的表观解离常数:静电校正。

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PURPOSE: Potentiometric lipid membrane-water partition coefficient studies neglect electrostatic interactions to date; this leads to incorrect results. We herein show how to account properly for such interactions in potentiometric data analysis. MATERIALS AND METHODS: We conducted potentiometric titration experiments to determine lipid membrane-water partition coefficients of four illustrative drugs, bupivacaine, diclofenac, ketoprofen and terbinafine. We then analyzed the results conventionally and with an improved analytical approach that considers Coulombic electrostatic interactions. RESULTS: The new analytical approach delivers robust partition coefficient values. In contrast, the conventional data analysis yields apparent partition coefficients of the ionized drug forms that depend on experimental conditions (mainly the lipid-drug ratio and the bulk ionic strength). This is due to changing electrostatic effects originating either from bound drug and/or lipid charges. A membrane comprising 10 mol-% mono-charged molecules in a 150 mM (monovalent) electrolyte solution yields results that differ by a factor of 4 from uncharged membranes results. CONCLUSION: Allowance for the Coulombic electrostatic interactions is a prerequisite for accurate and reliable determination of lipid membrane-water partition coefficients of ionizable drugs from potentiometric titration data. The same conclusion applies to all analytical methods involving drug binding to a surface.
机译:目的:电位脂质膜-水分配系数研究迄今忽略了静电相互作用。这会导致错误的结果。我们在这里展示了如何在电位数据分析中适当考虑这种相互作用。材料与方法:我们进行了电位滴定实验,以确定四种示例性药物布比卡因,双氯芬酸,酮洛芬和特比萘芬的脂质膜-水分配系数。然后,我们以常规方式和考虑了库仑静电相互作用的改进分析方法对结果进行了分析。结果:新的分析方法可提供可靠的分配系数值。相比之下,常规数据分析得出的离子化药物形式的表观分配系数取决于实验条件(主要是脂质-药物比率和整体离子强度)。这是由于源于结合的药物和/或脂质电荷的静电效应发生变化。在150 mM(单价)电解质溶液中包含10 mol%单电荷分子的膜所产生的结果与不带电荷的膜结果相差4倍。结论:库仑静电相互作用的允许是从电位滴定数据准确可靠地确定可离子化药物的脂质膜-水分配系数的先决条件。相同的结论适用于涉及药物与表面结合的所有分析方法。

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