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Targeting autophagy in disease: established and new strategies

AutorKocak, Muhammed; Ezazi Erdib, Saba; Jorba, Guillem; Maestro, Inés CSIC ORCID; Farrés, Judith; Kirkin, Vladimir; Martínez Gil, Ana CSIC ORCID ; Pless, Ole
Palabras claveAutophagy activators
Autophagy inhibitors
Autophagy modulators
Clinical trials
Drug discovery
Fecha de publicación9-jul-2021
EditorTaylor & Francis
CitaciónAutophagy (2021)
ResumenMacroautophagy/autophagy is an evolutionarily conserved pathway responsible for clearing cytosolic aggregated proteins, damaged organelles or invading microorganisms. Dysfunctional autophagy leads to pathological accumulation of the cargo, which has been linked to a range of human diseases, including neurodegenerative diseases, infectious and autoimmune diseases and various forms of cancer. Cumulative work in animal models, application of genetic tools and pharmacologically active compounds, has suggested the potential therapeutic value of autophagy modulation in disease, as diverse as Huntington, Salmonella infection, or pancreatic cancer. Autophagy activation versus inhibition strategies are being explored, while the role of autophagy in pathophysiology is being studied in parallel. However, the progress of preclinical and clinical development of autophagy modulators has been greatly hampered by the paucity of selective pharmacological agents and biomarkers to dissect their precise impact on various forms of autophagy and cellular responses. Here, we summarize established and new strategies in autophagy-related drug discovery and indicate a path toward establishing a more efficient discovery of autophagy-selective pharmacological agents. With this knowledge at hand, modern concepts for therapeutic exploitation of autophagy might become more plausible.
Versión del editorhttps://doi.org/10.1080/15548627.2021.1936359
URIhttp://hdl.handle.net/10261/246981
DOI10.1080/15548627.2021.1936359
ISSN1554-8627
E-ISSN1554-8635
Aparece en las colecciones: (PTI Salud Global) Colección Especial COVID-19
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