Materials Map

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The Materials Map is an open tool for improving networking and interdisciplinary exchange within materials research. It enables cross-database search for cooperation and network partners and discovering of the research landscape.

The dashboard provides detailed information about the selected scientist, e.g. publications. The dashboard can be filtered and shows the relationship to co-authors in different diagrams. In addition, a link is provided to find contact information.

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The Materials Map is still under development. In its current state, it is only based on one single data source and, thus, incomplete and contains duplicates. We are working on incorporating new open data sources like ORCID to improve the quality and the timeliness of our data. We will update Materials Map as soon as possible and kindly ask for your patience.

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in Cooperation with on an Cooperation-Score of 37%

Topics

Publications (1/1 displayed)

  • 2023Common mouse models of tauopathy reflect early but not late human disease30citations

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Cheng, Long
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Connors, Theresa R.
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Zalm, Patrick Van
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Hyman, Bradley
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2023

Co-Authors (by relevance)

  • Cheng, Long
  • Connors, Theresa R.
  • Zalm, Patrick Van
  • Hyman, Bradley
  • Viode, Arthur
  • Steen, Hanno
  • Bannon, Anthony
  • Chang, Rui
  • Dellovade, Tammy
  • Langlois, Xavier
  • Schlaffner, Christoph
  • Wenger, Kathrin
  • Renard, Bernhard
  • Oakley, Derek
OrganizationsLocationPeople

article

Common mouse models of tauopathy reflect early but not late human disease

  • Cheng, Long
  • Connors, Theresa R.
  • Zalm, Patrick Van
  • Hyman, Bradley
  • Rappsilber, Juri
  • Viode, Arthur
  • Steen, Hanno
  • Bannon, Anthony
  • Chang, Rui
  • Dellovade, Tammy
  • Langlois, Xavier
  • Schlaffner, Christoph
  • Wenger, Kathrin
  • Renard, Bernhard
  • Oakley, Derek
Abstract

<jats:title>Abstract</jats:title><jats:sec><jats:title>Background</jats:title><jats:p>Mouse models that overexpress human mutant Tau (P301S and P301L) are commonly used in preclinical studies of Alzheimer’s Disease (AD) and while several drugs showed therapeutic effects in these mice, they were ineffective in humans. This leads to the question to which extent the murine models reflect human Tau pathology on the molecular level.</jats:p></jats:sec><jats:sec><jats:title>Methods</jats:title><jats:p>We isolated insoluble, aggregated Tau species from two common AD mouse models during different stages of disease and characterized the modification landscape of the aggregated Tau using targeted and untargeted mass spectrometry-based proteomics. The results were compared to human AD and to human patients that suffered from early onset dementia and that carry the P301L Tau mutation.</jats:p></jats:sec><jats:sec><jats:title>Results</jats:title><jats:p>Both mouse models accumulate insoluble Tau species during disease. The Tau aggregation is driven by progressive phosphorylation within the proline rich domain and the C-terminus of the protein. This is reflective of early disease stages of human AD and of the pathology of dementia patients carrying the P301L Tau mutation. However, Tau ubiquitination and acetylation, which are important to late-stage human AD are not represented in the mouse models.</jats:p></jats:sec><jats:sec><jats:title>Conclusion</jats:title><jats:p>AD mouse models that overexpress human Tau using risk mutations are a suitable tool for testing drug candidates that aim to intervene in the early formation of insoluble Tau species promoted by increased phosphorylation of Tau.</jats:p></jats:sec>

Topics
  • impedance spectroscopy
  • mass spectrometry
  • size-exclusion chromatography
  • spectrometry