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Study of the pathological functions of mutant Tau proteins

Stage Master 2 - Equipe "Neurocytoskeleton Dynamics and Structure"

Stage / Eq I.Arnal et A.Andrieux

Objectifs

The main objectives of this project are 1) to determine how mutations on Tau proteins affect its interactions with microtubules, 2) to evaluate how such pathological variants of Tau alter the physiological functions of WT non-mutated Tau.

Résumé

In neurons, microtubules are involved in key cellular functions such as axonal transport and synaptic plasticity. Tau is a major neuronal microtubule-associated protein that also interacts with actin and regulates microtubule–actin crosstalk. In many neurodegenerative disorders collectively known as tauopathies, Tau undergoes abnormal modifications that lead to cytoskeletal defects. A major challenge in understanding tau toxicity is elucidating the molecular mechanisms by which pathological forms of Tau disrupt cytoskeletal organization. In this context, the aim of this internship is to determine how Tau mutations alter its ability to regulate microtubules and whether pathological Tau variants affect the physiological functions of wild-type (WT) Tau. To address these questions, biomimetic assays and single-molecule approaches will be used to reconstitute cytoskeletal networks from purified proteins. This "Learning-by-Building" approach will enable us to decipher the molecular mechanisms underlying the cytoskeletal defects induced by pathological Tau variants in neuronal cells.

Méthodes

Protein expression (bacteria) and purification (chromatography, affinity), co-sedimentation assays, SDS-PAGE. Bio-mimetic assays. Imaging (video-microscopy, TIRF) and image analysis (ImageJ).

Références

* Prezel et al. (2018) Tau can switch microtubule network organizations: from random networks to dynamic and stable bundles. Molecular Biology of the Cell 29(2):154–165. doi: 10.1091/mbc.E17-06-0429.
* Stoppin-Mellet et al. (2020) Studying Tau-Microtubule interaction using single-molecule TIRF microscopy. Methods Mol Biol 2101:77-91
* Fourest-Lieuvin et al. (2023) Controlled Tau cleavage in cells reveals abnormal localizations of Tau fragments. Neuroscience 518:162-177.

Domaines d'expertise requis

Cytoskeleton ; Protein biochemistry ; Fluorescence microscopy ; Data analysis

Contact

Virginie Stoppin-Mellet, enseignante-chercheuse UGA
Email : virginie.stoppin-melletatuniv-grenoble-alpes.fr (virginie[dot]stoppin-mellet[at]univ-grenoble-alpes[dot]fr)

Téléchargement

Offre de stage M2 2026-2027 (PDF, 208.51 Ko)

Contacts

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Publié le 16 juillet 2026

Mis à jour le 16 juillet 2026