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Annotation


Wegorzewska I, Bell S, Cairns NJ, Miller TM, Baloh RH. TDP-43 mutant transgenic mice develop features of ALS and frontotemporal lobar degeneration. Proc Natl Acad Sci U S A. 2009 Nov 3;106(44):18809-14. PubMed Abstract

  
Comments on Paper and Primary News
  Primary News: Meet the First Published TDP-43 Mouse

Comment by:  Samir Kumar-Singh
Submitted 16 October 2009  |  Permalink Posted 16 October 2009

This study elegantly gives a first insight on a transgenic mouse model of mutant TDP-43 (A315T) identified in familial ALS patients. For those in the field, it is clear that generating these mouse models is a mammoth task on its own. Among the many interesting findings in this paper, the first to catch my attention was that the 25-kDa TDP-43 C-terminal fragments (CTFs) were recovered from detergent-soluble fractions but not from urea fractions as observed in sporadic and familial ALS/FTLD patients. If the TDP-43 25-kDa CTFs would indeed be confirmed as the real culprit, this would yet again emphasize the importance of soluble but not aggregated protein/peptide in cellular toxicity, as has been shown for a number of other proteinopathies including Aβ, α-synuclein, polyglutamine expansion in Huntingtin, and mutant SOD1.

Another important observation made in this paper was that ubiquitin-immunoreactive (ir) inclusions observed in select neurons including motor neurons were not TDP-43-ir. Thus, the mutant TDP-43 (A315T) mice do not completely model ALS, where ubiquitin-ir...  Read more

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REAGENTS/MATERIAL:
Primary antibodies included anti-FLAG (1:500) (Sigma); rabbit anti-TDP-43 recognizing amino acids 1–260 (ProteinTech Group); rabbit anti-TDP-43 recognizing the C-terminal amino acids 350–414 (Novus); mouse monoclonal anti-ubiquitin (Ubi-1) (Chemicon); rabbit anti-GFAP (Dako); anti-synuclein and anti-PHF1 (gifts from Paul Kotzbauer, Washington University); mouse monoclonal anti-neurofilament H (SMI-32) (Covance, 1:500) and anti-CD11b (Serotec).

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