Literature DB >> 33352744

A Monoclonal Antibody against the C-Terminal Domain of Bacillus cereus Hemolysin II Inhibits HlyII Cytolytic Activity.

Natalia Rudenko1, Alexey Nagel2, Anna Zamyatina1,3, Anna Karatovskaya1, Vadim Salyamov2, Zhanna Andreeva-Kovalevskaya2, Alexander Siunov2, Alexander Kolesnikov2, Anna Shepelyakovskaya1, Khanafiy Boziev1, Bogdan Melnik4, Fedor Brovko1, Alexander Solonin2.   

Abstract

Bacillus cereus is the fourth most common cause of foodborne illnesses that produces a variety of pore-forming proteins as the main pathogenic factors. B. cereus hemolysin II (HlyII), belonging to pore-forming β-barrel toxins, has a C-terminal extension of 94 amino acid residues designated as HlyIICTD. An analysis of a panel of monoclonal antibodies to the recombinant HlyIICTD protein revealed the ability of the antibody HlyIIC-20 to inhibit HlyII hemolysis. A conformational epitope recognized by HlyIIC-20 was found. by the method of peptide phage display and found that it is localized in the N-terminal part of HlyIICTD. The HlyIIC-20 interacted with a monomeric form of HlyII, thus suppressing maturation of the HlyII toxin. Protection efficiencies of various B. cereus strains against HlyII were different and depended on the epitope amino acid composition, as well as, insignificantly, on downstream amino acids. Substitution of L324P and P324L in the hemolysins ATCC14579T and B771, respectively, determined the role of leucine localized to the epitope in suppressing the hemolysis by the antibody. Pre-incubation of HlyIIC-20 with HlyII prevented the death of mice up to an equimolar ratio. A strategy of detecting and neutralizing the toxic activity of HlyII could provide a tool for monitoring and reducing B. cereus pathogenicity.

Entities:  

Keywords:  ELISA; bacteriophage display; epitope mapping; hemolysis; hybridoma; in vivo efficiency; neutralizing monoclonal antibody; oligomerization; pore-forming toxin

Mesh:

Substances:

Year:  2020        PMID: 33352744      PMCID: PMC7767301          DOI: 10.3390/toxins12120806

Source DB:  PubMed          Journal:  Toxins (Basel)        ISSN: 2072-6651            Impact factor:   4.546


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