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The cyclic cystine ladder in θ-defensins is important for structure and stability, but not antibacterial activity

机译:θ-防御素中的环状胱氨酸阶梯对结构和稳定性很重要,但对抗菌活性不重要

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摘要

θ-Defensins are ribosomally synthesized cyclic peptides found in the leukocytes of some primate species and have promising applications as antimicrobial agents and scaffolds for peptide drugs. The cyclic cystine ladder motif, comprising a cyclic peptide backbone and three parallel disulfide bonds, is characteristic of θ-defensins. In this study, we explore the role of the cyclic peptide backbone and cystine ladder in the structure, stability, and activity of θ-defensins. θ-Defensin analogues with different numbers and combinations of disulfide bonds were synthesized and characterized in terms of their NMR solution structures, serum and thermal stabilities, and their antibacterial and membrane-binding activities. Whereas the structures and stabilities of the peptides were primarily dependent on the number and position of the disulfide bonds, their antibacterial and membrane-binding properties were dependent on the cyclic backbone. The results provide insights into the mechanism of action of θ-defensins and illustrate the potential of θ-defensin analogues as scaffolds for peptide drug design.
机译:θ-防御素是在某些灵长类动物的白细胞中发现的核糖体合成的环状肽,作为肽类药物的抗菌剂和支架具有广阔的应用前景。包含环肽骨架和三个平行二硫键的环状胱氨酸阶梯基序是θ-防御素的特征。在这项研究中,我们探索了环肽主链和胱氨酸阶梯在θ-防御素的结构,稳定性和活性中的作用。合成了具有不同数量和二硫键组合的θ-防御素类似物,并根据其NMR溶液结构,血清和热稳定性以及它们的抗菌和膜结合活性对其进行了表征。肽的结构和稳定性主要取决于二硫键的数量和位置,而其抗菌和膜结合特性则取决于环状骨架。结果提供了对θ-防御素作用机理的见解,并说明了θ-防御素类似物作为肽药物设计支架的潜力。

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