Literature DB >> 33194795

Caprine Bactenecins as Promising Tools for Developing New Antimicrobial and Antitumor Drugs.

Pavel M Kopeikin1, Maria S Zharkova1, Alexander A Kolobov2, Maria P Smirnova2, Maria S Sukhareva1, Ekaterina S Umnyakova1, Vladimir N Kokryakov1, Dmitriy S Orlov1, Boris L Milman1, Sergey V Balandin3, Pavel V Panteleev3, Tatiana V Ovchinnikova3,4, Aleksey S Komlev1, Alessandro Tossi5, Olga V Shamova1.   

Abstract

Proline-rich antimicrobial peptides (PR-AMPs) having a potent antimicrobial activity predominantly toward Gram-negative bacteria and negligible toxicity toward host cells, are attracting attention as new templates for developing antibiotic drugs. We have previously isolated and characterized several bactenecins that are promising in this respect, from the leukocytes of the domestic goat Capra hircus: ChBac5, miniChBac7.5N-α, and -β, as well as ChBac3.4. Unlike the others, ChBac3.4 shows a somewhat unusual pattern of activities for a mammalian PR-AMP: it is more active against bacterial membranes as well as tumor and, to the lesser extent, normal cells. Here we describe a SAR study of ChBac3.4 (RFRLPFRRPPIRIHPPPFYPPFRRFL-NH2) which elucidates its peculiarities and evaluates its potential as a lead for antimicrobial or anticancer drugs based on this peptide. A set of designed structural analogues of ChBac3.4 was explored for antibacterial activity toward drug-resistant clinical isolates and antitumor properties. The N-terminal region was found to be important for the antimicrobial action, but not responsible for the toxicity toward mammalian cells. A shortened variant with the best selectivity index toward bacteria demonstrated a pronounced synergy in combination with antibiotics against Gram-negative strains, albeit with a somewhat reduced ability to inhibit biofilm formation compared to native peptide. C-terminal amidation was examined for some analogues, which did not affect antimicrobial activity, but somewhat altered the cytotoxicity toward host cells. Interestingly, non-amidated peptides showed a slight delay in their impact on bacterial membrane integrity. Peptides with enhanced hydrophobicity showed increased toxicity, but in most cases their selectivity toward tumor cells also improved. While most analogues lacked hemolytic properties, a ChBac3.4 variant with two additional tryptophan residues demonstrated an appreciable activity toward human erythrocytes. The variant demonstrating the best tumor/nontumor cell selectivity was found to more actively initiate apoptosis in target cells, though its action was slower than that of the native ChBac3.4. Its antitumor effectiveness was successfully verified in vivo in a murine Ehrlich ascites carcinoma model. The obtained results demonstrate the potential of structural modification to manage caprine bactenecins' selectivity and activity spectrum and confirm that they are promising prototypes for antimicrobial and anticancer drugs design.
Copyright © 2020 Kopeikin, Zharkova, Kolobov, Smirnova, Sukhareva, Umnyakova, Kokryakov, Orlov, Milman, Balandin, Panteleev, Ovchinnikova, Komlev, Tossi and Shamova.

Entities:  

Keywords:  antibacterial activity; antibiofilm activity; antibiotics; antitumor activity; bactenecins; proline-rich antimicrobial peptides; structure–activity relationship; synergy

Year:  2020        PMID: 33194795      PMCID: PMC7604311          DOI: 10.3389/fcimb.2020.552905

Source DB:  PubMed          Journal:  Front Cell Infect Microbiol        ISSN: 2235-2988            Impact factor:   5.293


  80 in total

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