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首页> 外文期刊>Journal of Medicinal Chemistry >Ligands and Receptors with Broad Binding Capabilities Have Common Structural Characteristics: An Antibiotic Design Perspective
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Ligands and Receptors with Broad Binding Capabilities Have Common Structural Characteristics: An Antibiotic Design Perspective

机译:具有宽带结合能力的配体和受体具有共同的结构特征:抗生素设计视角

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摘要

The spread of antibiotic resistance is one of the most serious global public-health problems. Here we show that a particular class of homomers with binding sites spanning multiple protein chains is particularly suitable for targeting by broad-spectrum antibacterial agents because due to the slow evolutionary change of such binding pockets, ligands of such homomers are much more likely to bind their homologs than ligands of monomers, or homomers with a single-chain binding site. Additionally, using de novo ligand design and deep learning, we show that the chemical compounds that can bind several different receptors have common structural characteristics and that halogens and fragments similar to the building blocks existing antimicrobials are overrepresented in them. Finally, we show that binding multiple receptors selects for flexible compounds, which are less likely to accumulate in Gram-negative bacteria; thus there is trade-off between reducing the emergence of resistance by multitargeting and broad-spectrum antibacterial activity.
机译:抗生素耐药性的蔓延是全球最严重的公共卫生问题之一。在这里,我们表明,特定的类结合部位跨越多个蛋白质链同聚体是特别适合于广谱抗菌剂靶向,因为由于这样的结合口袋的缓慢进化改变,例如同聚体的配位体更加容易得多绑定自己同源物比单体的配体,或与单链结合位点同聚体。另外,使用从头配体设计和深度学习,我们表明,可结合多种不同的受体的化学化合物具有类似于积木现有抗微生物剂在其中过表达共同的结构特性和卤素和片段。最后,我们示出了用于灵活的化合物该绑定多种受体选择,这是不太可能在革兰氏阴性细菌累加;因此存在折衷由multitargeting和广谱的抗菌活性降低耐药性的出现之间。

著录项

  • 来源
    《Journal of Medicinal Chemistry 》 |2019年第21期| 共18页
  • 作者单位

    Univ Edinburgh Inst Genet &

    Mol Med MRC Human Genet Unit Crewe Rd Edinburgh EH4 2XU Midlothian Scotland;

    Univ Edinburgh Inst Genet &

    Mol Med MRC Human Genet Unit Crewe Rd Edinburgh EH4 2XU Midlothian Scotland;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学 ;
  • 关键词

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