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A Mutant ataxin-3 fragment results from processing at a site N-terminal to amino acid 190 in brain of Machado-Joseph disease-like transgenic mice

  • Veronica F. Colomer Gouldc(Author)
    ,
  • Daniel Gotib(Author)
    ,
  • Donna Pearcec(Author)
    ,
  • Guillermo A. Gonzalezc(Author)
    ,
  • Hong Gaoc(Author)
    ,
  • aAgency for Science, Technology and Research, Singapore
    ,
  • bDiagnostic Grifols Reagents R and D Division
    ,
  • cJohns Hopkins University
Research Output: Contribution to journal Article Peer-review

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Abstract

Machado-Joseph disease also called spinocerebellar ataxia type 3 (MJD/SCA3) is a hereditary and neurodegenerative movement disorder caused by ataxin-3 with a polyglutamine expansion (mutant ataxin-3). Neuronal loss in MJD/SCA3 is associated with a mutant ataxin-3 toxic fragment. Defining mutant ataxin-3 proteolytic site(s) could facilitate the identification of the corresponding enzyme(s). Previously, we reported a mutant ataxin-3 mjd1a fragment in the brain of transgenic mice (Q71) that contained epitopes C-terminal to amino acid 220. In this study, we generated and characterized neuroblastoma cells and transgenic mice expressing mutant ataxin-3 mjd1a lacking amino acids 190-220 (deltaQ71). Less deltaQ71 than Q71 fragments were detected in the cell but not mouse model. The transgenic mice developed an MJD/SCA3-like phenotype and their brain homogenates had a fragment containing epitopes C-terminal to amino acid 220. Our results support the toxic fragment hypothesis and narrow the mutant ataxin-3 cleavage site to the N-terminus of amino acid 190.

Publication Information

Output type

Research Output: Contribution to journal Article Peer-review

Original language

English

Pages from-to (Number of pages)

Pages 362-369 (8 pages)

Journal (Volume, Issue Number)

Neurobiology of Disease (Volume 27, Issue 3)

Publication milestones

  • Published - 01/09/2007

Publication status

Published - 01/09/2007

ISSN

0969-9961

External Publication IDs

  • Scopus: 34548329581
  • PubMed: 17632007
  • WOS: 000249638900012

Funding Details

FundersFunding numbers
NIH
NS42731-01
NCI
-
NINDS
R01NS042731
AHA
EIG 0140166N