Literature DB >> 31689387

Cre-inducible Adeno Associated Virus-mediated Expression of P301L Mutant Tau Causes Motor Deficits and Neuronal Degeneration in the Substantia Nigra.

Yang You1, Mina B Botros2, Alicia A Van Enoo3, Aaron Bockmiller4, Shawn Herron5, Jean Christophe Delpech6, Tsuneya Ikezu7.   

Abstract

Accumulation of microtubule associated protein tau in the substantia nigra is associated with several tauopathies including progressive supranuclear palsy (PSP). A number of studies have used mutant tau transgenic mouse model to mimic the neuropathology of tauopathies and disease phenotypes. However, tau expression in these transgenic mouse models is not specific to brain subregions, and may not recapitulate subcortical disease phenotypes of PSP. It is necessary to develop a new disease modeling system for cell and region-specific expression of pathogenic tau for modeling PSP in mouse brain. In this study, we developed a novel strategy to express P301L mutant tau to the dopaminergic neurons of substantia nigra by coupling tyrosine hydroxylase promoter Cre-driver mice with a Cre-inducible adeno-associated virus (iAAV). The results showed that P301L mutant tau was successfully transduced in the dopaminergic neurons of the substantia nigra at the presence of Cre recombinase and iAAV. Furthermore, the iAAV-tau-injected mice displayed severe motor deficits including impaired movement ability, motor balance, and motor coordination compared to the control groups over a short time-course. Immunochemical analysis revealed that tau gene transfer significantly resulted in loss of tyrosine hydroxylase-positive dopaminergic neurons and elevated phosphorylated tau in the substantia nigra. Our development of dopaminergic neuron-specific neurodegenerative mouse model with tauopathy will be helpful for studying the underlying mechanism of pathological protein propagation as well as development of new therapies.
Copyright © 2019 IBRO. Published by Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  adeno-associated virus; microtubule-associated protein tau; neurodegenerative diseases; substantia nigra; tauopathies

Mesh:

Substances:

Year:  2019        PMID: 31689387      PMCID: PMC6898791          DOI: 10.1016/j.neuroscience.2019.10.001

Source DB:  PubMed          Journal:  Neuroscience        ISSN: 0306-4522            Impact factor:   3.590


  39 in total

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Authors:  Tinh N Luong; Holly J Carlisle; Amber Southwell; Paul H Patterson
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Authors:  Katrina Albert; Merja H Voutilainen; Andrii Domanskyi; T Petteri Piepponen; Sari Ahola; Raimo K Tuominen; Christopher Richie; Brandon K Harvey; Mikko Airavaara
Journal:  J Neurosci Res       Date:  2018-12-12       Impact factor: 4.164

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Authors:  Nicolas C Royo; Luk H Vandenberghe; Jing-Yuan Ma; Alisse Hauspurg; Liya Yu; Margaret Maronski; Julie Johnston; Marc A Dichter; James M Wilson; Deborah J Watson
Journal:  Brain Res       Date:  2007-11-17       Impact factor: 3.252

9.  The importance of tau phosphorylation for neurodegenerative diseases.

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Journal:  Front Neurol       Date:  2013-07-01       Impact factor: 4.003

10.  Expression of A152T human tau causes age-dependent neuronal dysfunction and loss in transgenic mice.

Authors:  Sumihiro Maeda; Biljana Djukic; Praveen Taneja; Gui-Qiu Yu; Iris Lo; Allyson Davis; Ryan Craft; Weikun Guo; Xin Wang; Daniel Kim; Ravikumar Ponnusamy; T Michael Gill; Eliezer Masliah; Lennart Mucke
Journal:  EMBO Rep       Date:  2016-03-01       Impact factor: 8.807

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Journal:  Mol Cell Neurosci       Date:  2020-10-08       Impact factor: 4.314

2.  Sowing the Seeds of Discovery: Tau-Propagation Models of Alzheimer's Disease.

Authors:  Benjamin J Bell; Medhinee M Malvankar; Carolyn Tallon; Barbara S Slusher
Journal:  ACS Chem Neurosci       Date:  2020-10-13       Impact factor: 4.418

3.  Wolframin-1-expressing neurons in the entorhinal cortex propagate tau to CA1 neurons and impair hippocampal memory in mice.

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Journal:  Sci Transl Med       Date:  2021-09-15       Impact factor: 17.956

  3 in total

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