Streptococcus suis bacteria are one of the most serious health problems for pigs and an emerging zoonotic agent in humans working in the swine industry. S. suis bacteria express capsular polysaccharides (CPS) a major bacterial virulence factor that define the serotypes. Oligosaccharides resembling the CPS of S. suis serotypes 2, 3, 9, and 14 have been synthesized, glycans related to serotypes 2 and 9 were placed on glycan array surfaces to screen blood from infected pigs. Lead antigens for the development of semi‐synthetic S. suis serotypes 2 and 9 glycoconjugate veterinary vaccines were identified in this way.
Malaria,
a mosquito-borne disease caused by
Plasmodium
species,
claims more than 400,000 lives globally each year. The increasing
drug resistance of the parasite renders the development of new anti-malaria
drugs necessary. Alternatively, better delivery systems for already
marketed drugs could help to solve the resistance problem. Herein,
we report glucose-based ultra-small gold nanoparticles (Glc-NCs) that
bind to cysteine-rich domains of
Plasmodium falciparum
surface proteins
.
Microscopy shows that Glc-NCs
bind specifically to extracellular and all intra-erythrocytic stages
of
P. falciparum
.
Glc-NCs
may be used as drug delivery agents as illustrated for ciprofloxacin,
a poorly soluble antibiotic with low antimalarial activity. Ciprofloxacin
conjugated to Glc-NCs is more water-soluble than the free drug and
is more potent. Glyco-gold nanoparticles that target cysteine-rich
domains on parasites may be helpful for the prevention and treatment
of malaria.
Acinetobacter baumannii is a opportunistic bacterial pathogen responsible for serious nosocomial infections that is becoming increasingly resistant against antibiotics. Capsular polysaccharides (CPS) that cover A. baumannii are a major virulence factor that play an important role in pathogenesis, are used to assign serotypes and provide the basis for vaccine development. Synthetic oligosaccharides resembling the CPS of A. baumannii 17978 were printed onto microarray slides and used to screen sera from patients infected with A. baumannii as well as a monoclonal mouse antibody (mAb C8). A synthetic oligosaccharide emerged from glycan array screening as lead for the development of a vaccine against A. baumannii 17978. Tetrasaccharide 20 is a key epitope for recognition by an antibody and is a vaccine lead.
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