Intracellular Trafficking SNARE Protein, Syntaxin-6, is a Modifier of Prion and Tau Pathogenesis in vivo and in Cellular Models

Elizabeth Hill
Mitali Patel
Juan M Ribes
Jacqueline Linehan
Fuquan Zhang
Michael Farmer
Tatiana Jakubcova
Shyma Hamdan
Andrew Tomlinson
Tiziana Ercolani
Christian Schmidt
Parvin Ahmed
George Thirlway
Silvia Purro
Fabio Argentina
Aline T Marinho
Emma Jones
Nicholas Kaye
Craig Fitzhugh
Rohan de Silva
Graham S Jackson
Sebastian Brandner
Peter Kloehn
John Collinge
Thomas J Cunningham
Simon Mead

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Abstract

Syntaxin-6, a SNARE protein involved in intracellular protein trafficking, is a proposed risk factor for sporadic prion disease, progressive supranuclear palsy and Alzheimer’s disease. However, no study has validated its functional role in these diseases, explored the disease stage at which it is acting nor its mechanism of action. Here, we show that syntaxin-6 acts at early stages of prion disease in experimental mice by increasing disease transmission risk following inoculation with low prion doses. Conversely, syntaxin-6 does not affect prion propagation kinetics or toxicity during established disease. Syntaxin-6 manipulation in cellular models profoundly alters the subcellular distribution and morphologies of disease-related PrP and modifies prion export. Furthermore, syntaxin-6 knockout in a transgenic tauopathy mouse model exerts protective effects on numerous physiological, behavioural and neuropathological outcome measures. Therefore, our studies firmly establish syntaxin-6 as a modifier of prion and tau pathogenesis, providing key insights into a fundamental mechanism of neurodegeneration.

Version published to 10.1101/2025.02.19.635172v1 on bioRxiv
Feb 20, 2025

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