| Literature DB >> 36188342 |
Adrian Najer1,2, Joshua Blight2, Catherine B Ducker2, Matteo Gasbarri3, Jonathan C Brown4, Junyi Che1, Håkon Høgset1, Catherine Saunders1, Miina Ojansivu5, Zixuan Lu1, Yiyang Lin1, Jonathan Yeow1, Omar Rifaie-Graham1, Michael Potter1, Renée Tonkin1, Jelle Penders1, James J Doutch6, Athina Georgiadou4, Hanna M G Barriga5, Margaret N Holme5, Aubrey J Cunnington4, Laurence Bugeon2, Margaret J Dallman2, Wendy S Barclay4, Francesco Stellacci3,7, Jake Baum2, Molly M Stevens1,5.
Abstract
Infectious diseases continue to pose a substantial burden on global populations, requiring innovative broad-spectrum prophylactic and treatment alternatives. Here, we have designed modular synthetic polymer nanoparticles that mimic functional components of host cell membranes, yielding multivalent nanomimics that act by directly binding to varied pathogens. Nanomimic blood circulation time was prolonged by reformulating polymer-lipid hybrids. Femtomolar concentrations of the polymer nanomimics were sufficient to inhibit herpes simplex virus type 2 (HSV-2) entry into epithelial cells, while higher doses were needed against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Given their observed virustatic mode of action, the nanomimics were also tested with malaria parasite blood-stage merozoites, which lose their invasive capacity after a few minutes. Efficient inhibition of merozoite invasion of red blood cells was demonstrated both in vitro and in vivo using a preclinical rodent malaria model. We envision these nanomimics forming an adaptable platform for developing pathogen entry inhibitors and as immunomodulators, wherein nanomimic-inhibited pathogens can be secondarily targeted to sites of immune recognition.Entities:
Year: 2022 PMID: 36188342 PMCID: PMC9092191 DOI: 10.1021/acscentsci.1c01368
Source DB: PubMed Journal: ACS Cent Sci ISSN: 2374-7943 Impact factor: 18.728