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FRIMEDBIO-Fri prosj.st. med.,helse,biol

Defective mitophagy in Alzheimer Tau pathology: Mechanistic studies and AI-based drug development (‘AM-AI’)

Alternativ tittel: Defective mitophagy in Alzheimer Tau pathology: Mechanistic studies and AI-based drug development (‘AM-AI’)

Tildelt: kr 9,6 mill.

Alzheimers sykdom er den vanligste demensen og rammer rundt 35 millioner mennesker over hele verden. Det antydes at opphopning av "søppel" i hjernen (som Abeta-plakk og Tau-floker), på grunn av kompromittert "resirkulering", er en årsak til Alzheimers. Dette prosjektet har som mål å forstå hvorfor 'søppelbilen' slutter å virke ved Alzheimers sykdom. Når vi først forstår årsaken, kan vi bruke de moderne metodene, inkludert kostnadseffektiv kunstig intelligens, for å designe medikamentkandidater mot Alzheimers. Suksessen til dette prosjektet kan ha translasjonspotensial, og på lang sikt stor sosioøkonomisk innvirkning.

Alzheimer’s disease (AD), the most common form of dementia, affects over 35 million people worldwide and causes formidable economic challenges. Since 2003, over 250 drug candidates, predominantly targeting two pathological proteins: amyloid- (A) and Tau, have been tested in clinical trials for AD and have all failed. As such, there is a need to pursue new mechanistic studies in order to better understand the underlying causes of AD, and to discover new and effective drug targets. Mitochondria operate as cellular “powerhouses” and play a pivotal role in neuroplasticity and memory. Mitochondria are constantly exposed to stress and damage; thus, dysfunctional mitochondria must be efficiently eliminated via a cellular self-clearance system termed “mitophagy”. The Evandro F. Fang group at UiO is among the first groups to propose and demonstrate a causative role for defective mitophagy as a key driver in AD initiation and progression, and has demonstrated mitophagy induction as an effective way to inhibit memory loss in multiple AD animal models. However, the intricate mechanisms underlying the link between defective mitophagy in Tau pathology and how mitophagy induction inhibits the progression of p- Tau and NFTs are largely unknown. Here, we aim to test the hypothesis that ‘Impaired mitophagy in the entorhinal cortex (EC) contributes to initiation and progression of Tau pathology in AD’, and based on the new drug target ‘impaired mitophagy’ to identify potent neuronal mitophagy inducers for use as anti-AD drug candidates via an artificial intelligence (AI)-based approach. Understanding the mechanisms underlying defective mitophagy and its roles in AD may revolutionise our understanding of AD aetiology and propel clinical drug discovery in new and fruitful directions.

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FRIMEDBIO-Fri prosj.st. med.,helse,biol

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