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Tetrasaccharide iteration synthesis of a heparin-like dodecasaccharide and radiolabelling for in vivo tissue distribution studies

机译:肝素样十二糖的四糖迭代合成和放射性标记用于体内组织分布研究

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摘要

Heparin-like oligosaccharides mediate numerous important biological interactions, of which many are implicated in various diseases. Synthetic improvements are central to the development of such oligosaccharides as therapeutics and, in addition, there are no methods to elucidate the pharmacokinetics of structurally defined heparin-like oligosaccharides. Here we report an efficient two-cycle [4+4+4] tetrasaccharide-iteration-based approach for rapid chemical synthesis of a structurally defined heparin-related dodecasaccharide, combined with the incorporation of a latent aldehyde tag, unmasked in the final step of chemical synthesis, providing a generic end group for labelling/conjugation. We exploit this latent aldehyde tag for 3H radiolabelling to provide the first example of this kind of agent for monitoring in vivo tissue distribution and in vivo stability of a biologically active, structurally defined heparin related dodecasaccharide. Such studies are critical for the development of related saccharide therapeutics, and the data here establish that a biologically active, synthetic, heparin-like dodecasaccharide provides good organ distribution, and serum lifetimes relevant to developing future oligosaccharide therapeutics.
机译:肝素样寡糖介导许多重要的生物相互作用,其中许多与多种疾病有关。合成的改进对于诸如治疗剂的寡糖的开发至关重要,此外,还没有任何方法阐明结构确定的肝素样寡糖的药代动力学。在这里,我们报告了一种有效的两周期[4 + 4 + 4]四糖迭代为基础的方法,用于快速化学合成结构定义的肝素相关的十二糖,并结合了潜在的醛标记,在最终步骤中未进行掩盖。化学合成,为标记/偶联提供通用的端基。我们利用这种潜在的醛标记进行 3 H放射性标记,以提供这种试剂的第一个实例,用于监测生物活性,结构确定的肝素相关十二糖的体内组织分布和体内稳定性。此类研究对于相关糖类疗法的发展至关重要,此处的数据表明,具有生物学活性的合成肝素样十二糖具有良好的器官分布,并且血清寿命与开发未来的寡糖疗法有关。

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