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Deep mutational scanning and machine learning uncover antimicrobial peptide features driving membrane selectivity

biorxiv. 2023-09; 
Justin R. Randall; Luiz C. Vieira; Claus O. Wilke; Bryan W. Davies
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Peptide Synthesis libraries under investigation reported as log2-fold change scores. Peptide synthesis. All peptides used in this work were synthesized commercially by GenScript s custom peptide synthesis service and analyzed by RP-HPLC and mass spectrometry to confirm molecular weight. For high purity peptides (> 90%) final Get A Quote

摘要

Antimicrobial peptides commonly act by disrupting bacterial membranes, but also frequently damage mammalian membranes. Deciphering the rules governing membrane selectivity is critical to understanding their function and enabling their therapeutic use. Past attempts to decipher these rules have failed because they cannot interrogate adequate peptide sequence variation. To overcome this problem, we develop deep mutational surface localized antimicrobial display (dmSLAY), which reveals comprehensive positional residue importance and flexibility across an antimicrobial peptide sequence. We apply dmSLAY to Protegrin-1, a potent yet toxic antimicrobial peptide, and identify thousands of sequence variants that positiv... More

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