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用体内近红外荧光成像测量单糖-白蛋白缀合物的生物分布和排泄。

Biodistribution and excretion of monosaccharide-albumin conjugates measured with in vivo near-infrared fluorescence imaging.

机构信息

Molecular Imaging Program, Center for Cancer Research, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892-1088, USA.

出版信息

Bioconjug Chem. 2010 Oct 20;21(10):1925-32. doi: 10.1021/bc100313p.

Abstract

Target specific small molecules as modulators of drug delivery may play a significant role in the future development of therapeutics. Small molecules can alter the in vivo pharmacokinetics of therapeutic macromolecules leading to more efficient drug delivery with less systemic toxicity. The potential of creating a more effective drug delivery system through glycosylation has led, for instance, to the addition of galactose to increase drug delivery to the liver. However, there are many other monosaccharides with potentially useful targeting properties that require further characterization. Here, we investigate the potential of glycosylation to guide molecular therapies using five different monosaccharides conjugated to human serum albumin (HSA). Additionally, we investigate how the amount of glycosylation may alter the pharmacokinetic profile of HSA. We introduce the use of in vivo near-infrared optical imaging to characterize the effect of differential glycosylation on the pharmacokinetics of macromolecules.

摘要

靶向特定的小分子作为药物传递的调节剂,可能在未来治疗学的发展中发挥重要作用。小分子可以改变治疗性大分子的体内药代动力学,从而以较低的系统毒性实现更有效的药物传递。通过糖基化来创建更有效的药物传递系统的潜力,例如,已经导致向药物中添加半乳糖以增加药物向肝脏的传递。然而,还有许多其他具有潜在有用靶向特性的单糖需要进一步表征。在这里,我们使用五种不同的单糖与人血清白蛋白(HSA)缀合,研究了糖基化指导分子治疗的潜力。此外,我们还研究了糖基化的数量如何改变 HSA 的药代动力学特征。我们引入了体内近红外光学成像的使用,以描述差异糖基化对大分子药代动力学的影响。

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