Human Serum Albumin Grafted by Monomeric and Polymeric β-Cyclodextrin as Drug Delivery System for Levofloxacin with Improved Pharmacological Properties

T. Kopnova, L. R. Yakupova, N. G. Belogurova, E. V. Kudryashova
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Abstract

Human serum albumin (HSA) is a multifunctional protein, known to be a natural carrier for a number of endogenous and exogenous compounds, including drugs. HSA-based drugs formulation is a clinically validated approach to improve pharmacological properties and biodistribution (such as in Abraxane). Based on this, one might like to modify HSA in a way that its distribution is more favorable for certain therapeutic purposes. Levofloxacin (LV), a broad-spectrum antibiotic drug, could benefit from extended systemic exposure, and stronger interactions with plasma proteins could be useful for this purpose. We engrafted monomeric or polymeric cyclodextrins (CDs) on the surface of HSA molecules to strengthen the LV adsorption (the CD−LV dissociation constant is three orders of magnitude lower than that of HSA−LV). We found that (HSA−HPolS)conj+LV exhibited the highest activity against E. coli, whereas (HSA−HPCD)conj+LV was the most effective against B. subtilis, and both HSA conjugates were more potent than LV alone or LV with HSA. Further fine-tuning of HSA could yield an improvement in biodistribution and thus a more favorable risk/benefit ratio.
单体和聚合β-环糊精接枝的人血清白蛋白作为左氧氟沙星的给药系统,药理特性得到改善
人血清白蛋白(HSA)是一种多功能蛋白质,是包括药物在内的多种内源性和外源性化合物的天然载体。基于 HSA 的药物制剂是一种经过临床验证的改善药理特性和生物分布的方法(如 Abraxane)。在此基础上,人们可能希望对 HSA 进行改性,使其分布更有利于某些治疗目的。左氧氟沙星(LV)是一种广谱抗生素药物,它可以从扩大的全身暴露中获益,而与血浆蛋白更强的相互作用可能有助于实现这一目的。我们在 HSA 分子表面接枝了单体或聚合环糊精(CD),以加强对 LV 的吸附(CD-LV 的解离常数比 HSA-LV 低三个数量级)。我们发现(HSA-HPolS)conj+LV对大肠杆菌的活性最高,而(HSA-HPCD)conj+LV对枯草杆菌最有效,两种HSA共轭物都比单独的LV或含有HSA的LV更有效。进一步微调 HSA 可改善生物分布,从而获得更有利的风险/效益比。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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