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一种具有双向抗菌活性的新型富含色氨酸肽的溶液结构

Solution structure of a novel tryptophan-rich peptide with bidirectional antimicrobial activity.

作者信息

Wei Shu-Yi, Wu Jiun-Ming, Kuo Yen-Ya, Chen Heng-Li, Yip Bak-Sau, Tzeng Shiou-Ru, Cheng Jya-Wei

机构信息

Pacgen Biopharmaceuticals Corp., 1730-505 Burrard Street, Vancouver, BC V7X 1M6, Canada.

出版信息

J Bacteriol. 2006 Jan;188(1):328-34. doi: 10.1128/JB.188.1.328-334.2006.

DOI:10.1128/JB.188.1.328-334.2006
PMID:16352849
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1317575/
Abstract

Trp-rich antimicrobial peptides play important roles in the host innate defense mechanisms of many plants, insects, and mammals. A new type of Trp-rich peptide, Ac-KWRRWVRWI-NH(2), designated Pac-525, was found to possess improved activity against both gram-positive and -negative bacteria. We have determined that the solution structures of Pac-525 bound to membrane-mimetic sodium dodecyl sulfate (SDS) micelles. The SDS micelle-bound structure of Pac-525 adopts an alpha-helical segment at residues Trp2, Arg3, and Arg4. The positively charged residues are clustered together to form a hydrophilic patch. The three hydrophobic residues Trp2, Val6, and Ile9 form a hydrophobic core. The surface electrostatic potential map indicates the three tryptophan indole rings are packed against the peptide backbone and form an amphipathic structure. Moreover, the reverse sequence of Pac-525, Ac-IWRVWRRWK-NH(2), designated Pac-525(rev), also demonstrates similar antimicrobial activity and structure in membrane-mimetic micelles and vesicles. A variety of biophysical and biochemical methods, including circular dichroism, fluorescence spectroscopy, and microcalorimetry, were used to show that Pac-525 interacted strongly with negatively charged phospholipid vesicles and induced efficient dye release from these vesicles, suggesting that the antimicrobial activity of Pac-525 may be due to interactions with bacterial membranes.

摘要

富含色氨酸的抗菌肽在许多植物、昆虫和哺乳动物的宿主天然防御机制中发挥着重要作用。一种新型的富含色氨酸的肽,Ac-KWRRWVRWI-NH₂,命名为Pac-525,被发现对革兰氏阳性菌和阴性菌均具有增强的活性。我们已经确定了Pac-525与膜模拟物十二烷基硫酸钠(SDS)胶束结合的溶液结构。Pac-525与SDS胶束结合的结构在色氨酸2、精氨酸3和精氨酸4残基处采用α-螺旋片段。带正电荷的残基聚集在一起形成一个亲水区。三个疏水残基色氨酸2、缬氨酸6和异亮氨酸9形成一个疏水核心。表面静电势图表明,三个色氨酸吲哚环靠在肽主链上并形成一个两亲结构。此外,Pac-525的反向序列,Ac-IWRVWRRWK-NH₂,命名为Pac-525(rev),在膜模拟胶束和囊泡中也表现出类似的抗菌活性和结构。使用了多种生物物理和生化方法,包括圆二色性、荧光光谱和微量量热法,来表明Pac-525与带负电荷的磷脂囊泡强烈相互作用,并诱导这些囊泡有效地释放染料,这表明Pac-525的抗菌活性可能归因于与细菌膜的相互作用。

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