| Literature DB >> 30078314 |
Annachiara Gandini1,2, Manuela Bartolini1, Daniele Tedesco1, Loreto Martinez-Gonzalez3, Carlos Roca3, Nuria E Campillo3, Josefa Zaldivar-Diez3, Concepción Perez4, Giampaolo Zuccheri1,5, Andrea Miti1,5, Alessandra Feoli6, Sabrina Castellano6, Sabrina Petralla1, Barbara Monti1, Martina Rossi2, Fabio Moda7, Giuseppe Legname2, Ana Martinez3, Maria Laura Bolognesi1.
Abstract
Several findings propose the altered tau protein network as an important target for Alzheimer's disease (AD). Particularly, two points of pharmacological intervention can be envisaged: inhibition of phosphorylating tau kinase GSK-3β and tau aggregation process. On the basis of this consideration and on our interest in multitarget paradigms in AD, we report on the discovery of 2,4-thiazolidinedione derivatives endowed with such a profile. 28 and 30 displayed micromolar IC50 values toward GSK-3β, together with the capacity of inhibiting AcPHF6 aggregation of 60% and 80% at 10 μM, respectively. In addition, they showed PAMPA-BBB permeability, together with a suitable cellular safety profile. 30 also displayed inhibition of both K18 and full-length tau aggregations. Finally, both compounds were able to improve cell viability in an okadaic acid-induced neurodegeneration cell model. To the best of our knowledge, 28 and 30 are the first balanced, nontoxic, dual-acting compounds hitting tau cascade at two different hubs.Entities:
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Year: 2018 PMID: 30078314 DOI: 10.1021/acs.jmedchem.8b00610
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446