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三缬菌素 GA IV:一种用于新型缩氨酸抗生素合成的多功能模板。

Trichogin GA IV: a versatile template for the synthesis of novel peptaibiotics.

机构信息

ICB, Padova Unit, CNR, Department of Chemistry, University of Padova, 35131, Padova, Italy.

出版信息

Org Biomol Chem. 2012 Feb 14;10(6):1285-99. doi: 10.1039/c1ob06178j. Epub 2011 Dec 19.

Abstract

Trichogin GA IV, isolated from the fungus Trichoderma longibrachiatum, is the prototype of lipopeptaibols, the sub-class of short-length peptaibiotics exhibiting membrane-modifying properties. This peptaibol is predominantly folded in a mixed 3(10)-/α- helical conformation with a clear, albeit modest, amphiphilic character, which is likely to be responsible for its capability to perturb bacterial membranes and to induce cell death. In previous papers, we reported on the interesting biological properties of trichogin GA IV, namely its good activity against Gram positive bacteria, in particular methicillin-resistant S. aureus strains, its stability towards proteolytic degradation, and its low hemolytic activity. Aiming at broadening the antimicrobial activity spectrum by increasing the peptide helical amphiphilicity, in this work we synthesized, by solution and solid-phase methodologies, purified and fully characterized a set of trichogin GA IV analogs in which the four Gly residues at positions 2, 5, 6, 9, lying in the poorly hydrophilic face of the helical structure, are substituted by one (position 2, 5, 6 or 9), two (positions 5 and 6), three (positions 2, 5, and 9), and four (positions 2, 5, 6, and 9) Lys residues. The conformational preferences of the Lys-containing analogs were assessed by FT-IR absorption, CD and 2D-NMR techniques in aqueous, organic, and membrane-mimetic environments. Interestingly, it turns out that the presence of charged residues induces a transition of the helical conformation adopted by the peptaibols (from 3(10)- to α-helix) as a function of pH in a reversible process. The role played in the analogs by the markedly increased amphiphilicity was further tested by fluorescence leakage experiments in model membranes, protease resistance, antibacterial and antifungal activities, cytotoxicity, and hemolysis. Taken together, our biological results provide evidence that some of the least substituted among these analogs are good candidates for the development of new membrane-active antimicrobial agents.

摘要

从长梗木霉中分离得到的 Trichogin GA IV 是脂肽菌素的原型,是具有膜修饰特性的短肽菌素的亚类。这种肽菌素主要以混合 3(10)-/α-螺旋构象折叠,具有明显但适度的两亲性,这可能是其扰乱细菌膜并诱导细胞死亡的能力的原因。在以前的论文中,我们报道了 Trichogin GA IV 的有趣生物学特性,即其对革兰氏阳性菌,特别是耐甲氧西林的金黄色葡萄球菌菌株的良好活性,对蛋白水解降解的稳定性以及低溶血活性。为了通过增加肽的螺旋两亲性来拓宽抗菌活性谱,在这项工作中,我们通过溶液和固相方法合成、纯化并充分表征了一组 Trichogin GA IV 类似物,其中四个位于螺旋结构疏水面的 Gly 残基(位置 2、5、6、9)被一个(位置 2、5、6 或 9)、两个(位置 5 和 6)、三个(位置 2、5 和 9)和四个(位置 2、5、6 和 9)Lys 残基取代。通过在水相、有机相和膜模拟环境中的 FT-IR 吸收、CD 和 2D-NMR 技术评估了含 Lys 类似物的构象偏好。有趣的是,结果表明,带电荷残基的存在会诱导肽菌素所采用的螺旋构象发生转变(从 3(10)-到α-螺旋),这是一个在可逆过程中随 pH 值变化的过程。在模型膜中通过荧光泄漏实验、蛋白酶抗性、抗菌和抗真菌活性、细胞毒性和溶血实验进一步测试了类似物中明显增加的两亲性所起的作用。综上所述,我们的生物学结果表明,这些类似物中取代最少的一些是开发新型膜活性抗菌剂的良好候选物。

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