Abstract
Heat-stable enterotoxin (ST) producing enterotoxigenic Escherichia coli (ETEC) strains are among the top four enteropathogens associated with moderate-to-severe diarrhea in children under five years in low-to-middle income countries, thus making ST a target for an ETEC vaccine. However, ST must be mutated to abolish its enterotoxicity and to prevent a potential immunological cross-reaction due to its structural resemblance to the human peptides uroguanylin and guanylin. To reduce the risk of eliciting cross-reacting antibodies with our lead STh-A14T toxoid, L9 was chosen as an additional mutational target. A double mutant vaccine candidate immunogen, STh-L9A/A14T, was constructed by conjugation to the synthetic virus-like mi3 nanoparticle using the SpyTag/SpyCatcher technology. This immunogen elicited STh neutralizing antibodies in mice, but with less consistency than STh-A14T peptide control immunogens. Moreover, individual sera from mice immunized with both single and double mutant variants displayed varying levels of unwanted cross-reacting antibodies. The lowest levels of cross-reacting antibodies were observed with STh-L9K/A14T control immunogens, suggesting that it is indeed possible to reduce the risk of eliciting cross-reacting antibodies by mutation. However, mutant-specific antibodies were observed for most double mutant immunogens, demonstrating the delicate balancing act between disrupting cross-reacting epitopes, keeping protective ones, and avoiding the formation of neoepitopes.
Highlights
Enterotoxigenic Escherichia coli (ETEC) infection accounts for over 50,000 human deaths annually [1]
Heat-stable enterotoxin (ST) producing enterotoxigenic Escherichia coli (ETEC) strains are among the top four enteropathogens associated with moderate-to-severe diarrhea in children under five years in low-to-middle income countries, making ST a target for an ETEC vaccine
Colonization allows ST-producing ETEC (ST-ETEC) to effectively deliver ST to the intestinal guanylyl cyclase C (GC-C) receptor, prompting a signaling cascade that leads to the disruption of water and electrolyte homeostasis, which may lead to a profuse watery diarrhea
Summary
Enterotoxigenic Escherichia coli (ETEC) infection accounts for over 50,000 human deaths annually [1]. ETEC represents a genetically diverse group of E. coli strains defined by the secretion of heat-stable enterotoxin (ST) and/or heat-labile enterotoxin (LT). ST-ETEC infection increases the risk of death in children younger than 24 months with MSD [4], as well as contributing to long-term sequelae associated with diarrhea in these children [5,6]. Colonization allows ST-ETEC to effectively deliver ST to the intestinal guanylyl cyclase C (GC-C) receptor, prompting a signaling cascade that leads to the disruption of water and electrolyte homeostasis, which may lead to a profuse watery diarrhea. ETEC strains infecting humans can carry either or both of two subtypes of ST, namely the 19-amino acid human ST (STh) and the 18-amino acid porcine ST (STp) [11,12]. STh and STp share 14 amino acids and have highly similar structures due to three shared structure-defining disulfide bonds [11,13]
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