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Ω76: A designed antimicrobial peptide to combat carbapenem- and tigecycline-resistant

Sci Adv. 2019-07-01; 
Deepesh Nagarajan, Natasha Roy, Omkar Kulkarni, Neha Nanajkar, Akshay Datey, Sathyabaarathi Ravichandran, Chandrani Thakur, Sandeep T, Indumathi V Aprameya, Siddhartha P Sarma, Dipshikha Chakravortty, Nagasuma Chandra
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Peptide Synthesis … The sequence alignment was done using ClustalW36. The alignment images were generated using Seaview37. Protein structures have been superimposed using MUSTANG38. In vitro Synthesized chemical peptides were obtained from GenScript USA, Inc … Get A Quote

摘要

Drug resistance is a public health concern that threatens to undermine decades of medical progress. ESKAPE pathogens cause most nosocomial infections, and are frequently resistant to carbapenem antibiotics, usually leaving tigecycline and colistin as the last treatment options. However, increasing tigecycline resistance and colistin's nephrotoxicity severely restrict use of these antibiotics. We have designed antimicrobial peptides using a maximum common subgraph approach. Our best peptide (Ω76) displayed high efficacy against carbapenem and tigecycline-resistant in mice. Mice treated with repeated sublethal doses of Ω76 displayed no signs of chronic toxicity. Sublethal Ω76 doses co-administered alongside s... More

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