| Literature DB >> 32176482 |
Laura M De Plano1, Santina Carnazza1, Domenico Franco1, Maria Giovanna Rizzo1, Sabrina Conoci2,3, Salvatore Petralia2, Alessandra Nicoletti4, Mario Zappia4, Michela Campolo1, Emanuela Esposito1, Salvatore Cuzzocrea1, Salvatore P P Guglielmino1.
Abstract
An innovative approach to identify new conformational antigens of Aβ1-42 recognized by IgG autoantibodies as biomarkers of state and stage in Alzheimer's disease (AD) patients is described. In particular, through the use of bioinformatics modeling, conformational similarities between several Aβ1-42 forms and other amyloid-like proteins with F1 capsular antigen (Caf1) of Yersinia pestis were first found. pVIII M13 phage display libraries were then screened against YPF19, anti-Caf1 monoclonal antibody, and IgGs of AD patients, in alternate biopanning cycles of a so-called "double binding" selection. From the selected phage clones, one, termed 12III1, was found to be able to prevent in vitro Aβ1-42-induced cytotoxicity in SH-SY5Y cells, as well as to promote disaggregation of preformed fibrils, to a greater extent with respect to wild-type phage (pC89). IgG levels detected by 12III1 provided a significant level of discrimination between diseased and nondemented subjects, as well as a good correlation with the state progression of the disease. These results give significant impact in AD state and stage diagnosis, paving the way for the development not only for an innovative blood diagnostic assay for AD precise diagnosis, progressive clinical assessment, and screening but also for new effective treatments.Entities:
Keywords: AD state and stage progression screening; Aβ1−42 cytotoxicity inhibition; Phage display double binding selection; amyloid conformational epitopes; autoantibody detection; fibril disaggregation
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Year: 2020 PMID: 32176482 PMCID: PMC7997372 DOI: 10.1021/acschemneuro.9b00549
Source DB: PubMed Journal: ACS Chem Neurosci ISSN: 1948-7193 Impact factor: 4.418