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Evento

1-Mesytil-3-(3-sulfonatopropyl)imidazolium protects against oxidative stress and delyas proteotoxicity in C. elegans

Andersen, Natalia DeniseIcon ; Veuthey, Tania VanesaIcon ; Blanco, Maria GabrielaIcon ; Silbestri, Gustavo FabiánIcon ; Rayes, Diego HernánIcon ; de Rosa, Maria JoseIcon
Tipo del evento: Congreso
Nombre del evento: 24th International C. elegans Conference
Fecha del evento: 24/06/2023
Institución Organizadora: Genetics Society of America;
Título del Libro: Libro de resumenes: 24th International C. elegans Conference
Editorial: Genetics Society of America
Idioma: Inglés
Clasificación temática:
Biología Celular, Microbiología

Resumen

Due to the increase in life expectancy, age-related neurodegenerative diseases (NDs) have become more prevalent. Conventional treatments fail to arrest or delay neuronal proteotoxicity that characterizes these diseases. Due to their diverse biological activities, imidazole rings are intensively explored as powerful scaffolds for the development of new bioactive molecules. By using C. elegans, our work aims to explore novel biological roles for these compounds. To this end, we have tested the in vivo anti-proteotoxic effects of imidazolium salts. Since NDs have been largely linked to impaired antioxidant defense mechanisms, we focused on 1-Mesityl-3-(3-sulfonatopropyl) imidazolium (MSI), one of the imidazolium salts that we identified as capable of improving iron-induced oxidative stress resistance in wild-type animals. By combining mutant and gene expression analysis we have determined that this protective effect depends on the activation of the Heat Shock Transcription Factor (HSF1), whereas it is independent of other canonical cytoprotective molecules such as abnormal Dauer Formation-16 (DAF-16/ FOXO) and Skinhead-1 (SKN-1/Nrf2). To delve deeper into the biological roles of MSI, we analyzed its impact on previously established C. elegans models of protein aggregation. We found that MSI ameliorates β-amyloid-induced paralysis in worms expressing the pathological protein involved in Alzheimer’s Disease. Moreover, MSI also delays age-related locomotion decline in other proteotoxic C. elegans models, suggesting a broad protective effect. Taken together, our results point to MSI as a promising anti-proteotoxic compound and provide proof of concept of the potential of imidazole derivatives in the development of novel therapies to retard age-related proteotoxic diseases.
Palabras clave: C. ELEGANS , INVERTEBRADOS , PROTEOSTASIS , OXIDATIVE STRESS
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info:eu-repo/semantics/openAccess Excepto donde se diga explícitamente, este item se publica bajo la siguiente descripción: Creative Commons Attribution-NonCommercial-ShareAlike 2.5 Unported (CC BY-NC-SA 2.5)
Identificadores
URI: http://hdl.handle.net/11336/221894
URL: https://genetics-gsa.org/celegans2023/
URL: https://genetics-gsa.org/celegans2023/program-and-abstract-books/
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Eventos(INIBIBB)
Eventos de INST.DE INVEST.BIOQUIMICAS BAHIA BLANCA (I)
Citación
1-Mesytil-3-(3-sulfonatopropyl)imidazolium protects against oxidative stress and delyas proteotoxicity in C. elegans; 24th International C. elegans Conference; Glasgow; Reino Unido; 2023; 475-475
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