Development of novel antimicrobials with engineered endolysin LysECD7-SMAP to combat Gram-negative bacterial infections

Author:

Vasina Daria V.ORCID,Antonova Nataliia P.,Gushchin Vladimir A.,Aleshkin Andrey V.,Fursov Mikhail V.,Fursova Anastasiia D.,Gancheva Petya G.,Grigoriev Igor V.,Grinkevich Pavel,Kondratev Alexey V.,Kostarnoy Alexey V.,Lendel Anastasiya M.,Makarov Valentine V.,Nikiforova Maria A.,Pochtovyi Andrei A.,Prudnikova Tatiana,Remizov Timofey A.,Shevlyagina Natalia V.,Siniavin Andrei E.,Smirnova Nina S.,Terechov Alexander A.,Tkachuk Artem P.,Usachev Evgeny V.,Vorobev Aleksei M.,Yakimakha Victoria S.,Yudin Sergey M.,Zackharova Anastasia A.,Zhukhovitsky Vladimir G.,Logunov Denis Y.,Gintsburg Alexander L.

Abstract

Abstract Background Among the non-traditional antibacterial agents in development, only a few targets critical Gram-negative bacteria such as carbapenem-resistant Pseudomonas aeruginosa, Acinetobacter baumannii or cephalosporin-resistant Enterobacteriaceae. Endolysins and their genetically modified versions meet the World Health Organization criteria for innovation, have a novel mode of antibacterial action, no known bacterial cross-resistance, and are being intensively studied for application against Gram-negative pathogens. Methods The study presents a multidisciplinary approach, including genetic engineering of LysECD7-SMAP and production of recombinant endolysin, its analysis by crystal structure solution following molecular dynamics simulations and evaluation of antibacterial properties. Two types of antimicrobial dosage forms were formulated, resulting in lyophilized powder for injection and hydroxyethylcellulose gel for topical administration. Their efficacy was estimated in the treatment of sepsis, and pneumonia models in BALB/c mice, diabetes-associated wound infection in the leptin receptor-deficient db/db mice and infected burn wounds in rats. Results In this work, we investigate the application strategies of the engineered endolysin LysECD7-SMAP and its dosage forms evaluated in preclinical studies. The catalytic domain of the enzyme shares the conserved structure of endopeptidases containing a putative antimicrobial peptide at the C-terminus of polypeptide chain. The activity of endolysins has been demonstrated against a range of pathogens, such as Klebsiella pneumoniae, A. baumannii, P. aeruginosa, Staphylococcus haemolyticus, Achromobacter spp, Burkholderia cepacia complex and Haemophylus influenzae, including those with multidrug resistance. The efficacy of candidate dosage forms has been confirmed in in vivo studies. Some aspects of the interaction of LysECD7-SMAP with cell wall molecular targets are also discussed. Conclusions Our studies demonstrate the potential of LysECD7-SMAP therapeutics for the systemic or topical treatment of infectious diseases caused by susceptible Gram-negative bacterial species and are critical to proceed LysECD7-SMAP-based antimicrobials trials to advanced stages.

Funder

Centre for Strategic Planning and Management of Biomedical Health Risks of the Federal Medical Biological Agency

Publisher

Springer Science and Business Media LLC

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