Synthesis and Structure?Activity Relationship Studies of N?Terminal Analogues of the Antimicrobial Peptide Tridecaptin A1

Stephen A. Cochrane; Christopher T. Lohans; Jeremy R. Brandelli; George Mulvey; Glen D. Armstrong; John C. Vederas

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Synthesis and Structure?Activity Relationship Studies of N?Terminal Analogues of the Antimicrobial Peptide Tridecaptin A1

机译：抗菌肽十三烷A1 N末端类似物的合成与结构-活性关系研究

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Chemical synthesis was used to increase the potency of the antimicrobial lipopeptide tridecaptin A1. Lipid tail modification proved to be an ideal platform for synthesizing structurally simpler analogues that are not readily accessible by isolation. The stereochemical elements of the tridecaptin A1 lipid tail are not essential for antimicrobial activity and could be replaced with hydrophobic aliphatic or aromatic groups. Some simpler analogues displayed potent antimicrobial activity against Gram-negative bacteria, including Campylobacter jejuni, Escherichia coli O157:H7, and multidrug resistant Klebsiella pneumoniae.

机译：化学合成被用来增加抗菌脂肽十三烷A1的效力。脂质尾部修饰被证明是合成结构简单的类似物的理想平台，这些类似物不易通过分离获得。 Tridecaptin A1脂质尾部的立体化学元素对于抗菌活性不是必需的，可以被疏水性脂族或芳族基团取代。一些更简单的类似物显示出对革兰氏阴性细菌有效的抗菌活性，包括空肠弯曲菌，大肠杆菌O157：H7和耐多药肺炎克雷伯菌。

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《Journal of Medicinal Chemistry》 |2014年第3期|共5页
作者
Stephen A. Cochrane; Christopher T. Lohans; Jeremy R. Brandelli; George Mulvey; Glen D. Armstrong; John C. Vederas;
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正文语种 eng
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关键词
Synthesis; Structure?Activity; Relationship Studies;

机译：合成;结构活性;关系研究;

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1. Synthesis and Structure?Activity Relationship Studies of N?Terminal Analogues of the Antimicrobial Peptide Tridecaptin A1 [J] . Stephen A. Cochrane, Christopher T. Lohans, Jeremy R. Brandelli, Journal of Medicinal Chemistry . 2014,第3期

机译：抗菌肽十三烷A1 N末端类似物的合成与结构-活性关系研究
2. Combinatorial libraries: A tool to design antimicrobial and antifungal peptide analogues having lyric specificities for structure-activity relationship studies [J] . Blondelle SE., Lohner K. Biopolymers: Original Research on Biomolecules and Biomolecular Assemblies . 2000,第1期

机译：组合文库：设计具有抒情特异性的抗微生物和抗真菌肽类似物的工具，用于结构-活性关系研究
3. Antimicrobial Peptides with Potential for Biofilm Eradication: Synthesis and Structure Activity Relationship Studies of Battacin Peptides [J] . De Zoysa Gayan Heruka, Cameron Alan James, Hegde Veena V., Journal of Medicinal Chemistry . 2015,第2期

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4. SARP: A comprehensive design platform for studying structure-activity relationship of antimicrobial peptides [C] . Quhuan Li IT in Medicine and Education (ITME), 2011 International Symposium on . 2011

机译：SARP：研究抗菌肽结构-活性关系的综合设计平台
5. Peptoid mimics of helical, cationic antimicrobial peptides: Studies of structure-activity relationships, synergy, and mechanism. [D] . Chongsiriwatana, Nathaniel P. 2008

机译：螺旋，阳离子抗菌肽的类肽模拟物：结构活性关系，协同作用和机理的研究。
6. Structure-Activity Relationships of the Antimicrobial Peptide Arasin 1 — And Mode of Action Studies of the N-Terminal, Proline-Rich Region [O] . Victoria S. Paulsen, Hans-Matti Blencke, Monica Benincasa, 2010

机译：抗菌肽Arasin 1的构效关系-脯氨酸丰富区N端的作用方式研究
7. Structure-activity relationships of the antimicrobial peptide arasin 1 - and mode of action studies of the N-terminal, proline-rich region. [O] . Victoria S Paulsen, Hans-Matti Blencke, Monica Benincasa, 2013

机译：抗菌肽arasin 1的结构 - 活性关系 - 以及N末端，富含脯氨酸的区域的作用模式研究。

Synthesis and Structure?Activity Relationship Studies of N?Terminal Analogues of the Antimicrobial Peptide Tridecaptin A1

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