Design Engineering and Discovery of Novel α-Helical and β-Boomerang Antimicrobial Peptides against Drug Resistant Bacteria

机译：新型α - 螺旋和β-Boomerang抗微生物肽对耐药细菌的设计工程和发现

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In an era where the pipeline of new antibiotic development is drying up, the continuous rise of multi-drug resistant (MDR) and extensively drug resistant (XDR) bacteria are genuine threats to human health. Although antimicrobial peptides (AMPs) may serve as promising leads against drug resistant bacteria, only a few AMPs are in advanced clinical trials. The limitations of AMPs, namely their low in vivo activity, toxicity, and poor bioavailability, need to be addressed. Here, we review engineering of frog derived short α-helical AMPs (aurein, temporins) and lipopolysaccharide (LPS) binding designed β-boomerang AMPs for further development. The discovery of novel cell selective AMPs from the human proprotein convertase furin is also discussed.

机译：在新的抗生素发育的管道枯竭的时代，多毒性（MDR）的连续上升和广泛的毒性（XDR）细菌是对人类健康的真正威胁。虽然抗微生物肽（AMPS）可以作为对抗耐药细菌的有前途的导致，但只有少数AMPS正在进行晚期临床试验。 AMPS的局限性，即它们在体内活性，毒性和生物利用度不佳的低的局限性。在这里，我们审查青蛙衍生的短α-Helical AMPS（AUREIN，TIMALIN）和脂多糖（LPS）结合设计的β-BOOMERANG AMPS进行进一步发展。还讨论了来自人类proProtein转化酶Furin的新细胞选择性安培的发现。

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期刊名称 International Journal of Molecular Sciences
作者
Surajit Bhattacharjya; Suzana K. Straus;
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作者单位

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年(卷),期 2020(21),16
年度 2020
页码 -1
总页数 21
原文格式 PDF
正文语种
中图分类分子生物学;
关键词
multi-drug resistant (MDR) bacteria; extensively drug resistant (XDR) bacteria; antimicrobial peptides (AMPs); lipopolysaccharide (LPS) binding; α-helical and β-boomerang AMPs;

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专利

1. Cell-selectivity of tryptophan and tyrosine in amphiphilic α-helical antimicrobial peptides against drug-resistant bacteria [J] . Min-Young Lee, Seong-Cheol Park, Myunghwan Jung, Biochemical and Biophysical Research Communications . 2018,第2期

机译：耐药细菌抗药性α-螺旋抗微生物肽中色氨酸和酪氨酸的细胞选择性
2. Disruption of drug-resistant biofilms using de novo designed short alpha-helical antimicrobial peptides with idealized facial amphiphilicity [J] . Khara Jasmeet Singh, Obuobi Sybil, Wang Ying, Acta biomaterialia . 2017,第期

机译：使用De Novo设计的短α-螺旋抗微生物肽具有理想化面部两亲性的耐药生物膜的破坏
3. Antibacterial activity of the recombinant antimicrobial peptide Ib-AMP4 from Impatiens balsamina and its synergy with other antimicrobial agents against drug resistant bacteria [J] . FanX., ReichlingJ., WinkM. Die Pharmazie . 2013,第7期

机译：凤仙花（Impatiens balsamina）重组抗菌肽Ib-AMP4的抗菌活性及其与其他抗菌剂的协同抗药性
4. Chemical modifications of short antimicrobial peptides from insects and vertebrates to fight multi-drug resistant bacteria [C] . Daniel Knappe, Ghristin Stegemann, Ariane Nimptsch American Peptide Symposium . 2009

机译：昆虫和脊椎动物短抗菌肽的化学修饰，对抗多药物抗菌细菌
5. The antimicrobial activity of proteins/peptides against antibiotic-resistant and -susceptible bacteria. [D] . Greiner, Laura Lee. 2001

机译：蛋白质/肽对抗生素耐药和易感细菌的抗菌活性。
6. Computational antimicrobial peptide design and evaluation against multidrug-resistant clinical isolates of bacteria [O] . Deepesh Nagarajan, Tushar Nagarajan, Natasha Roy, 2018

机译：计算性抗菌肽的设计和对细菌多药耐药临床分离株的评估
7. Disruption of drug-resistant biofilms using de novo designed short α-helical antimicrobial peptides with idealized facial amphiphilicity [O] . Khara, JS, Obuobi, S, Wang, Y, 2017

机译：使用de novo设计的短α-螺旋抗菌肽破坏抗药性生物膜，具有理想化的面部两亲性

Design Engineering and Discovery of Novel α-Helical and β-Boomerang Antimicrobial Peptides against Drug Resistant Bacteria

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