Contribution to drug discovery and development for tauopathies using yeast as a model

Posted on:2016-07-18

Degree:Ph.D

Type:Dissertation

University:Universidade NOVA de Lisboa (Portugal)

Candidate:Cerejo, Marta Isabel Heitor

Full Text:PDF

GTID:1474390017480324

Subject:Pharmacology

Abstract/Summary:

This work aimed to contribute to drug discovery and development (DDD) for tauopathies, while expanding our knowledge on this group of neurodegenerative disorders, including Alzheimer's disease (AD). Using yeast, a recognized model for neurodegeneration studies, useful models were produced for the study of tau interaction with beta-amyloid (Abeta), both AD hallmark proteins. The characterization of these models suggests that these proteins co-localize and that Abeta1-42, which is toxic to yeast, is involved in tau40 phosphorylation (Ser396/404) via the GSK-3beta yeast orthologue, whereas tau seems to facilitate Abeta1-42 oligomerization. The mapping of tau's interactome in yeast, achieved with a tau toxicity enhancer screen using the yeast deletion collection, provided a novel framework, composed of 31 genes, to identify new mechanisms associated with tau pathology, as well as to identify new drug targets or biomarkers. This genomic screen also allowed to select the yeast strain mir1Delta-tau40 for development of a new GPSD2TM drug discovery screening system. A library of unique 138 marine bacteria extracts, obtained from the Mid-Atlantic Ridge hydrothermal vents, was screened with mir1Delta-tau40. Three extracts were identified as suppressors of tau toxicity and constitute good starting points for DDD programs. mir1Delta strain was sensitive to tau toxicity, relating tau pathology with mitochondrial function. SLC25A3, the human homologue of MIR1, codes for the mitochondrial phosphate carrier protein (PiC). Resorting to iRNA, SLC25A3 expression was silenced in human neuroglioma cells, as a first step towards the engineering of a neural model for replicating the results obtained in yeast. This model is essential to understand the mechanisms of tau toxicity at the mitochondrial level and to validate PiC as a relevant drug target. The set of DDD tools here presented will foster the development of innovative and efficacious therapies, urgently needed to cope with tau-related disorders of high human and social-economic impact.

Keywords/Search Tags:

Tau, Development, Drug discovery, Yeast, DDD, Using, Model

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