| Literature DB >> 29503604 |
Krystina L Hess1, Eunkeu Oh2, Lisa H Tostanoski1, James I Andorko1, Kimihiro Susumu2, Jeffrey R Deschamps3, Igor L Medintz3, Christopher M Jewell1.
Abstract
Treatments for autoimmunity - diseases where the immune system mistakenly attacks self-molecules - are not curative and leave patients immunocompromised. New studies aimed at more specific treatments reveal development of inflammation or tolerance is influenced by the form self-antigens are presented. Using a mouse model of multiple sclerosis (MS), we show for the first time that quantum dots (QDs) can be used to generate immunological tolerance by controlling the density of self-antigen on QDs. These assemblies display dense arrangements of myelin self-peptide associated with disease in MS, are uniform in size (<20 nm), and allow direct visualization in immune tissues. Peptide-QDs rapidly concentrate in draining lymph nodes, co-localizing with macrophages expressing scavenger receptors involved in tolerance. Treatment with peptide-QDs reduces disease incidence 10-fold. Strikingly, the degree of tolerance - and the underlying expansion of regulatory T cells - correlates with the density of myelin molecules presented on QDs. A key discovery is that higher numbers of tolerogenic particles displaying lower levels of self-peptide are more effective for inducing tolerance than fewer particles each displaying higher densities of peptide. QDs conjugated with self-antigens could serve as a new platform to induce tolerance, while visualizing QD therapeutics in tolerogenic tissue domains.Entities:
Keywords: autoimmunity; modeling and simulation; quantum dots and nanoparticles; theranostics; tolerance; vaccine and immunotherapy
Year: 2017 PMID: 29503604 PMCID: PMC5828250 DOI: 10.1002/adfm.201700290
Source DB: PubMed Journal: Adv Funct Mater ISSN: 1616-301X Impact factor: 18.808