| Literature DB >> 34095846 |
Harlei Martin1, Tara Somers2, Mathew Dwyer2, Ryan Robson3, Frederick M Pfeffer3, Ragnar Bjornsson4, Tobias Krämer1,5, Kevin Kavanagh2,6, Trinidad Velasco-Torrijos1,6.
Abstract
Candida albicans is one of the most prevalent fungal pathogens involved in hospital acquired infections. It binds to glycans at the surface of epithelial cells and initiates infection. This process can be blocked by synthetic carbohydrates that mimic the structure of cell surface glycans. Herein we report the evaluation of a series of divalent glycosides featuring aromatic (benzene, squaramide) and bicyclic aliphatic (norbornene) scaffolds, with the latter being the first examples of their kind as small molecule anti-adhesion glycoconjugates. Galactosides 1 and 6, built on an aromatic core, were most efficient inhibitors of adhesion of C. albicans to buccal epithelial cells, displacing up to 36% and 48%, respectively, of yeast already attached to epithelial cells at 138 μM. Remarkably, cis-endo-norbornene 21 performed comparably to benzene-core derivatives. Conformational analysis reveals a preference for compounds 1 and 21 to adopt folded conformations. These results highlight the potential of norbornenes as a new class of aliphatic scaffolds for the synthesis of anti-adhesion compounds. This journal is © The Royal Society of Chemistry.Entities:
Year: 2020 PMID: 34095846 PMCID: PMC8126883 DOI: 10.1039/d0md00224k
Source DB: PubMed Journal: RSC Med Chem ISSN: 2632-8682