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Home: Papers of the Week
Annotation


Redwine JM, Kosofsky B, Jacobs RE, Games D, Reilly JF, Morrison JH, Young WG, Bloom FE. Dentate gyrus volume is reduced before onset of plaque formation in PDAPP mice: a magnetic resonance microscopy and stereologic analysis. Proc Natl Acad Sci U S A. 2003 Feb 4;100(3):1381-6. PubMed Abstract

  
Comments on Paper and Primary News
  Primary News: Mutant AβPP Retards Growth in Hippocampus before Plaques Form

Comment by:  Mark Mattson, ARF Advisor
Submitted 23 January 2003  |  Permalink Posted 23 January 2003

The quantitative analyses of volumes of different brain structures in an APP mutant mouse line by Redwine et al. provide valuable new information concerning the possible relationships between altered APP processing, amyloid deposition, and cellular damage in Alzheimer's disease. The data reveal reductions in the size of the hippocampal dentate gyrus and the corpus callosum that occur prior to evidence of amyloid deposits. Indeed, both of these brain structures are smaller in the APP mutant mice as early as 40 days of age with further divergence from age-matched non-transgenic control mice at 100 days of age. Previous studies of this line of APP mutant mice have suggested no cell loss in the hippocampus, although numbers of dentate granule cells have not been quantified in a rigorous manner. However, there are data suggesting that numbers of synapses are decreased in APP mutant mice. It will be important to establish that similar decreases in the sizes of the dentate gyrus and corpus callosum occur in other lines of APP mutant transgenic mice, and to determine whether the...  Read more

  Primary News: Mutant AβPP Retards Growth in Hippocampus before Plaques Form

Comment by:  Paul Coleman, ARF Advisor
Submitted 28 January 2003  |  Permalink Posted 28 January 2003

This study by Redwine and colleagues is very well done and meticulous. It convincingly demonstrates reduced volume of the dentate gyrus by 100 days of age in the PDAPP transgenic mouse model of Alzheimer’s disease. Aβ-containing plaques have been shown to accumulate in this model by 240-300 days. Thus, this paper is crucial in demonstrating a frank, fairly gross structural change well in advance of the appearance of one of the major traditional markers of AD pathology.

It is important to note that two independent methods were used and that they both arrived at similar conclusions. Meticulous magnetic resonance microscopy (MRM) was used (T2 images, 11.7 T equipment) to determine the volumes of the total brain, hippocampus and cerebellum. Genu–splenium length of the corpus callosum was also measured. Ages studied were 40 days, 100 days, and 12 and 21 months. MRM data were obtained from perfusion-fixed mouse brains while still in the skull. Brain was then removed, sectioned at 50µm, and stained with thionin and cresyl violet. These stained sections were used to obtain unbiased...  Read more


  Primary News: Mutant AβPP Retards Growth in Hippocampus before Plaques Form

Comment by:  Scott Small
Submitted 5 February 2003  |  Permalink Posted 5 February 2003

When introduced as a clinical tool in the 1980s, MRI transformed the field of clinical neuroscience. Visualizing the brain with exquisite anatomical resolution was one thing, but to accomplish this feat noninvasively, so that human subjects could be imaged repeatedly over time, was too good to be true. Finally, we had a technique allowing us to study the natural course of disease in living patients. Up to that point, we’d relied mainly on dead human tissue, or if we wanted to study disease in a living system, we turned to animal models and used invasive mapping techniques. In a perfect illustration of science’s dialectical course, the current study—which is as powerful as it is elegant—shows that MRI’s utility can be retrofitted to the study of dead mice.

Why so much excitement over this seemingly retrogressive trend? One reason is that after a few decades of perfecting imaging protocols designed to highlight different aspects of brain anatomy and function, we now need to verify what it is we are actually imaging. Verification is best accomplished in animal models of disease...  Read more


  Primary News: Mutant AβPP Retards Growth in Hippocampus before Plaques Form

Comment by:  Gunnar K. Gouras
Submitted 10 February 2003  |  Permalink Posted 10 February 2003

The study by Redwine et al. provides important new evidence for FAD mutant AβPP and/or elevated Aβ causing preplaque structural changes in a well-established FAD transgenic mouse strain. The excellent comments on this paper reinforce the point that the study of how mutant APP/Aβ may relate to synaptic dysfunction and selective regional volume loss in brain certainly is an important area of study. A major question is how AβPP or Aβ is responsible for these changes. Increasing evidence favors a role for soluble Aβ oligomers in this pathological process (multiple studies; i.e., Walsh et al., 2002). Increasing evidence also indicates that preplaque Aβ accumulation occurs within nerve cells in FAD transgenic mice and AD brain (also, multiple studies, most recently Shie et al., 2003; see ARF online discussion). The biological interactions of these different pools of brain Aβ, especially...  Read more

  Comment by:  Todd E. Golde
Submitted 17 February 2003  |  Permalink Posted 17 February 2003
  I recommend this paper

The is an interesting and somewhat unexpected finding. At 100 days of age PDAPP mice show a small but significant decrease in hippocampal volume (12.3%). This is before there is measurable biochemical or immunohistochemical Abeta deposition. The main quesiton raised by this study is whether the change is due to APP, soluble Abeta, or even non-specific transgene effects. Further studies will be needed to sort out these possibilities.

View all comments by Todd E. Golde
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REAGENTS/MATERIAL:

Transgenic male PDAPP and WT (Taconic Farms)were used in this study.

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