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Home: Papers of the Week
Annotation


Kirik D, Rosenblad C, Burger C, Lundberg C, Johansen TE, Muzyczka N, Mandel RJ, Björklund A. Parkinson-like neurodegeneration induced by targeted overexpression of alpha-synuclein in the nigrostriatal system. J Neurosci. 2002 Apr 1;22(7):2780-91. PubMed Abstract

  
Comments on Paper and Primary News
  Primary News: Viral Transgenic Techniques Pay Off In Parkinson's Models

Comment by:  Ronald Klein
Submitted 3 April 2002  |  Permalink Posted 3 April 2002

While the germline transgenic approach is the gold standard for studying gene function in the brain, it is also labor-intensive, expensive, and requires long periods of time to screen and raise the animals. We have adopted an alternative somatic transgenic strategy (historically applied for gene therapy) where the mutant genes can be expressed directly in the brains of adult animals, a method that by comparison, is inexpensive and fast.

The application of a somatic-cell transgenic approach to modeling neurodegenerative diseases will be useful for several reasons, including: (1) temporal control of expression to avoid developmental effects and also to study aging effects, i.e. similar periods of expression in young or aged subjects; (2) spatial control of expression to target brain regions associated with specific disease states; and (3) transgene combinations.

Further, the vector-based approaches can be applied to rats or monkeys and also take advantage of internal controls, i.e. comparisons to the contralateral, untreated hemisphere. Despite some real limitations of this...  Read more


  Primary News: Viral Transgenic Techniques Pay Off In Parkinson's Models

Comment by:  Deniz Kirik
Submitted 3 April 2002  |  Permalink Posted 3 April 2002

I believe the most important aspect of our study is that we describe a new approach to study protein dysfunction in appropriate animal models with a strong basis in morphological, biochemical as well as behavioral assessments. Our model offers numerous advantages over transgenic mouse models. For example, it can easily be generated using wild-type animals in sufficient numbers with a very simple surgical intervention; the animals can be rendered transgenic at any time during their lifetime; it can be applied unilaterally leaving the contralateral side as an internal control; detailed functional assessments can better be done using rats as compared with mice; the model can be applied to primates to answer certain question that cannot be satisfactorily addressed in rodents.

The method is very reproducible. We have now done (including new experiments not included in this paper) over 500 surgeries, and in all cases we can hit nearly all of the nigral dopamine cells with very high precision. This model is unique because the AAV vectors have a high affinity to these cells.

As...  Read more


  Primary News: Viral Transgenic Techniques Pay Off In Parkinson's Models

Comment by:  Eliezer Masliah
Submitted 3 April 2002  |  Permalink Posted 3 April 2002

Use of viral vector for targeting transgene expression in a region- and time-specific manner was first demonstrated to model a neurodegenerative disorder, namely trinucleotide repeat disease, by Fred Gage's lab (Senut et al., 2000). This approach offers a unique opportunity for the development and modeling of neurodegenerative disorders in a rapid and reliable manner. It also offers a unique opportunity of testing in vivo selective neuronal vulnerability and the differential effects of mutations.

A similar approach is currently under development by our group in collaboration with Fred Gage and Inder Verma to model Alzheimer's disease and other neurodegenerative disorders using lentiviral vectors. This approach also holds great promise for the development of new treatments for PD.

View all comments by Eliezer Masliah

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REAGENTS/MATERIAL:

Immunohistochemical stainings were performed on free-floating sections using antibodies raised against TH (mouse IgG, 1:2000; Chemicon), GFP (chicken IgG, 1:5000; R & D systems), vesicular monoamine transporter-2 (VMAT-2) (rabbit IgG, 1:5000; Chemicon), Hu (mouse IgG, 1:1000; gift of Dr. Steven A. Goldman, Cornell University), and human a-synuclein (mouse IgG, 1:2000; courtesy of Dr. Virginia M. Lee, University of Pennsylvania).

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