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Diversity-Oriented A(3)-Macrocyclization for Studying Influences of Ring-Size and Shape of Cyclic Peptides: CD36 Receptor Modulators

机译:多样性导向的A(3)-大环化研究环状肽环大小和形状的影响:CD36受体调节剂

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摘要

Cyclic peptide diversity has been broadened by elaborating the A(3)-macrocyclization to include various di-amino carboxylate components with different N-epsilon-amine substituents. Triple-bond reduction provided new cyclic peptide macrocycles with Z-olefin and completely saturated structures. Moreover, cyclic azasulfurylpeptides were prepared by exchanging the propargylglycine (Pra) component for an amino sulfamide surrogate. Examination of such diversity-oriented methods on potent cyclic azapeptide modulators of the cluster of differentiation 36 receptor (CD36) identified the importance of the triple bond as well as the N-epsilon-allyl lysine and azaPra residues for high CD36 binding affinity. Cyclic azapeptides which engaged CD36 effectively reduced pro-inflammatory nitric oxide and downstream cytokine and chemokine production in macrophages stimulated with a Toll-like receptor-2 agonist. Studying the triple bond and amine components in the multiple-component A(3)-macrocyclization has given a diverse array of macrocycles and pertinent information to guide the development of ideal CD36 modulators with biomedical potential for curbing macrophage-driven inflammation.
机译:通过细化 A(3)-大环化,包括具有不同 N-ε-胺取代基的各种二氨基羧酸酯组分,环肽多样性得到了扩展。三键还原提供了具有Z-烯烃和完全饱和结构的新型环肽大环。此外,通过将炔丙基甘氨酸(Pra)组分交换为氨基磺酰胺替代物来制备环氮杂硫酰肽。对分化簇 36 受体 (CD36) 的强效环氮杂肽调节剂的这种多样性导向方法的检查确定了三键以及 N-ε-烯丙基赖氨酸和氮杂普拉残基对高 CD36 结合亲和力的重要性。参与 CD36 的环氮杂肽可有效减少 Toll 样受体-2 激动剂刺激的巨噬细胞中促炎一氧化氮以及下游细胞因子和趋化因子的产生。研究多组分 A(3)-大环化中的三键和胺组分提供了多种大环和相关信息,以指导开发具有抑制巨噬细胞驱动炎症的生物医学潜力的理想 CD36 调节剂。

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