| Literature DB >> 35997936 |
Cleonice Creusa Santos1, Thyago R Cardim-Pires2, Liana Shvachiy3,4, Luis Arturo Fonseca-Fonseca5, Patricia Muñoz6, Áurea Maria A N Almeida1, Ana Carla S Costa1, Jéssica Teles-Souza1, Estael Ochoa-Rodríguez7, Maria de Fátima Dias Costa1, Fernando L Palhano2, Juan Segura-Aguilar8, Deyse B Barbosa9, Mayra R do Bomfim9, Manoelito C Dos Santos Junior9, Franco Henrique A Leite9, Samuel Silva da Rocha Pita10, Silvia Lima Costa1, Yanier Núñez-Figueredo5, Tiago Fleming Outeiro3,11,12,13, Débora Foguel2, Victor Diogenes Amaral Silva14.
Abstract
Studies showed that JM-20, a benzodiazepine-dihydropyridine hybrid molecule, protects against rotenone and 6-hydroxydopamine neurotoxicity. However, its protective effects against cytotoxicity induced by endogenous neurotoxins involved in Parkinson's disease (PD) pathogenesis have never been investigated. In this study, we evaluated the ability of JM-20 to inhibit alpha-synuclein (aSyn) aggregation. We also evaluated the interactions of JM-20 with aSyn by molecular docking and molecular dynamics and assessed the protective effect of JM-20 against aminochrome cytotoxicity. We demonstrated that JM-20 induced the formation of heterogeneous amyloid fibrils, which were innocuous to primary cultures of mesencephalic cells. Moreover, JM-20 reduced the average size of aSyn positive inclusions in H4 cells transfected with SynT wild-type and synphilin-1-V5, but not in HEK cells transfected with synphilin-1-GFP. In silico studies showed the interaction between JM-20 and the aSyn-binding site. Additionally, we showed that JM-20 protects SH-SY5Y cells against aminochrome cytotoxicity. These results reinforce the potential of JM-20 as a neuroprotective compound for PD and suggest aSyn as a molecular target for JM-20.Entities:
Keywords: Alpha-synuclein; JM-20; Neuroprotection; Neurotoxicity; Parkinson’s disease
Year: 2022 PMID: 35997936 DOI: 10.1007/s12640-022-00559-7
Source DB: PubMed Journal: Neurotox Res ISSN: 1029-8428 Impact factor: 3.978