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Molecular Characterization of Mucus Binding

机译:粘液结合的分子表征

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摘要

Binding of small molecules to mucus membranes in the body has an important role in human health, as it can affect the diffusivity and activity of any molecule that acts in a mucosal environment. The binding of drugs and of toxins and signaling molecules from mucosal pathogens is of particular clinical interest. Despite the importance of mucus-small molecule binding, there is a lack of data revealing the precise chemical features of small molecules that lead to mucus binding. We developed a novel equilibrium dialysis assay to measure the binding of libraries of small molecules to mucin and other mucus components, substantially increasing the throughput of small molecule binding measurements. We validated the biological relevance of our approach by quantifying binding of the antibiotic colistin to mucin, and showing that this binding was associated with inhibition of colistin's bioactivity. We next used a small molecule microarray to identify 2,4-diaminopyrimidine as a mucin binding motif and confirmed the importance of this motif for mucin binding using equilibrium dialysis. Furthermore, we showed that, for molecules with this motif, binding to mucins and the mucus-associated biopolymers DNA and alginate is modulated by differences in hydrophobicity and charge. Finally, we showed that molecules lacking the motif exhibited different binding trends from those containing the motif. These results open up the prospect of routine testing of small molecule binding to mucus and optimization of drugs for clinically relevant mucus binding properties.
机译:小分子在体内的粘膜结合在人体健康中具有重要作用,因为它可以影响作用在粘膜环境中的任何分子的扩散和活性。药物和毒素和信号分子来自粘膜病原体的结合是特别的临床兴趣。尽管粘液小分子结合具有重要性,但缺乏缺乏导致粘液结合的小分子的精确化学特征。我们开发了一种新的平衡透析测定,以测量小分子文库对粘蛋白和其他粘液组分的结合,显着增加了小分子结合测量的吞吐量。我们通过量化抗生素Colistin与粘蛋白的结合来验证我们的方法的生物学相关性,并且表明该结合与抑制Colistin的生物活性有关。接下来使用小分子微阵列以鉴定2,4-二氨基嘧啶作为粘蛋白结合基序,并确认了使用平衡透析的粘液结合的本赛题的重要性。此外,我们表明,对于具有该基序的分子,与粘蛋白结合和粘液相关的生物聚合物DNA和藻酸盐通过疏水性和电荷的差异调节。最后,我们表明,缺乏图案的分子表现出与含有图案的那些具有不同的结合趋势。这些结果开辟了对粘液的小分子与粘液结合的常规测试的前景,以及用于临床相关的粘液结合性的药物的优化。

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  • 来源
    《Biomacromolecules》 |2019年第4期|共9页
  • 作者单位

    MIT Dept Biol Engn 77 Massachusetts Ave Cambridge MA 02139 USA;

    MIT Dept Biol Engn 77 Massachusetts Ave Cambridge MA 02139 USA;

    MIT Dept Biol Engn 77 Massachusetts Ave Cambridge MA 02139 USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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