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Mechanism of cholesterol gallstone dissolution. I. The determination of the binding of alkyl amines to bile micelles using dynamic membrane transport methods

机译:胆固醇胆结石溶解的机制。 I.使用动态膜输送方法测定烷基胺与胆汁胶束的结合

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摘要

Recent studies have shown that cholesterol monohydrate pellet dissolution rates in real and synthetic bile systems are enhanced dramatically in the presence of small concentrations of amines (primary, secondary, and tertiary), quaternary ammonium compounds, and cationic surfactants. These studies have shown that, in general, chain length, the degree of hydrophobicity, the ability to alter micellar charge, as well as the steric or structural features of these molecules seem to be important. In all of the past studies, however, the situations have been complicated by the fact that the accelerator molecules in question were bound to varying degrees to the micelles and other components of the synthetic bile. Meaningful structure activity relationships can only be considered when the concentrations of bound and unbound drug are known. A dynamic cellulose membrane dialysis technique was used; in evaluating the validity of the technique for the present purposes the following factors were considered: (a) the possible influence of membrane charge on dialysis, (b) the possible influence of bile acid-lecithin micelles on dialysis rate, (c) the possible influence of pore size and molecular structure on dialysis rate, and finally (d) the influence of Donnan membrane effects. Some of the results obtained using this technique were compared to the results obtained using the silicone rubber membrane system. There is very good agreement between the data obtained using the two methods. Thus, the good agreement underscores the validity of either method and rules out, for example, the possibility that an amine-chenodeoxycholate complex is being transported across either or both membranes.
机译:最近的研究表明,在小浓度的胺(初级,仲和叔),季铵化合物和阳离子表面活性剂的存在下,胆固醇单水合物沉淀率在实际和合成胆汁系统中具有显着提高。这些研究表明,通常,链长,疏水程度,改变胶束电荷的能力,以及这些分子的空间或结构特征似乎是重要的。然而,在所有过去的研究中,情况由于所讨论的促进剂分子与胶束和合成胆汁的其他组分相结合,所讨论的促进剂分子被变得复杂。当已知结束和未结合药物的浓度和未结合药物的浓度时,才能考虑有意义的结构活动关系。使用动态纤维素膜透析技术;在评估本发明的技术的有效性时,考虑了以下因素:(a)膜充电对透析的可能影响,(b)胆酸 - 卵磷脂胶束对透析率的可能影响,(c)可能的影响孔径和分子结构对透析率的影响,最后(d)唐南膜效应的影响。将使用该技术获得的一些结果与使用硅橡胶膜系统获得的结果进行比较。使用这两种方法获得的数据之间存在非常良好的一致性。因此,良好的协议强调了任一方法和规则的有效性,例如,胺 - 癸酸核素复合物在两种或两种膜上被运输的可能性。

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