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黑色素特性对药物结合特性的影响。

Influence of Melanin Characteristics on Drug Binding Properties.

机构信息

Roche Pharmaceutical Research and Early Development , Roche Innovation Center Basel , 4070 Basel , Switzerland.

School of Pharmacy , University of Eastern Finland , 70211 Kuopio , Finland.

出版信息

Mol Pharm. 2019 Jun 3;16(6):2549-2556. doi: 10.1021/acs.molpharmaceut.9b00157. Epub 2019 Apr 30.

Abstract

Melanins are biopolymers encompassing a high degree of chemical heterogeneity. Binding of small-molecule drugs to ocular melanin significantly affects the ocular pharmacokinetics, and could serve as a strategy for prolonged drug retention in the eye. The influence of the structural and physical characteristics of melanins originating from different sources on their drug binding properties has not yet been methodically investigated. We performed physical characterization of Sepia officinalis, synthetic and porcine melanin. The particle size distribution was analyzed by laser diffractometry. A dynamic vapor sorption method, requiring small amounts of the material, was developed to analyze the differences in the specific surface area of the melanins. The extent of melanin binding at equilibrium was determined for a set of 34 small-molecule drugs and compared across different melanin types. Despite systematic shifts in the extent of binding within a twofold range, binding data were highly correlated across the melanins. These moderate differences in binding could not be directly explained by the substantial differences in particle size and were more in line with the relatively similar specific surface area of these different melanin materials. Overall, these results suggest that the specific surface area reflects the actual accessibility of a small molecule in the melanin structure and could serve as a surrogate to explain the binding differences observed for the respective melanin materials.

摘要

黑色素是包含高度化学异质性的生物聚合物。小分子药物与眼部黑色素的结合显著影响眼部药代动力学,可作为延长药物在眼部滞留时间的策略。然而,源自不同来源的黑色素的结构和物理特性对其药物结合特性的影响尚未系统地研究过。我们对乌贼黑色素、合成黑色素和猪黑色素进行了物理特性分析。通过激光衍射法分析了粒径分布。开发了一种动态蒸汽吸附方法,该方法需要少量的材料,以分析黑色素比表面积的差异。确定了一组 34 种小分子药物在平衡时的黑色素结合程度,并在不同类型的黑色素之间进行了比较。尽管结合程度在两倍范围内存在系统变化,但黑色素之间的结合数据高度相关。这些结合的中等差异不能直接用粒径的显著差异来解释,而更符合这些不同黑色素材料相对相似的比表面积。总的来说,这些结果表明比表面积反映了小分子在黑色素结构中的实际可及性,并可以作为解释各自黑色素材料观察到的结合差异的替代指标。

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