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High yield synthesis of cyclic analogues of antibacterial peptides P-113 by Sortase A-mediated ligation and their conformation studies 被引量:2
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作者 Zhi-Meng Wu Shao-Zhong Liu +2 位作者 Xiao-Zhong Cheng Xin-Rui Zhao Hao-Fei Hong 《Chinese Chemical Letters》 SCIE CAS CSCD 2017年第3期553-557,共5页
P-113 is a fragment of natural occurring peptide Histatin 5 found in human saliva. This peptide exhibited broad spectrum of antibacterial and antifungal biological activities. In this study, bifunctional P-113 peptide... P-113 is a fragment of natural occurring peptide Histatin 5 found in human saliva. This peptide exhibited broad spectrum of antibacterial and antifungal biological activities. In this study, bifunctional P-113 peptides 2–5 were designed as Sortase A substrates and synthesized by solid support peptide synthesis,where the N-terminus were equipped with glycine and its analogues, and C-terminus were extended with LPETGGS, respectively. Under Sortase A catalyzed condition, head to tail cyclization products 7–10were afforded in yields from 76% to 93%. The conformation insights of linear peptides 2–5 and cyclic analogues 7–10 in aqueous buffers and in trifluroethanol(TFE) analyzed by circular dichroism(CD)suggested that a-helix structures were produced progressively in hydrophobic environment independent of the cyclization, which displayed the similar behavior as parent peptide P-113. 展开更多
关键词 Antibacterial peptide P-113 Cyclization Sortase a-mediated ligation Conformation Circular dichroism
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