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Evidence That Aging And Amyloid Promote Microglial Cell Senescence

Barry Flanary, Nicole W. Sammons, Cuong Thach Nguyen, Douglas G. Walker, Wolfgang J. Streit

Rejuvenation Research · 2007 · ▲ 273 citations

Abstract

Advanced age and presence of intracerebral amyloid deposits are known to be major risk factors for development of neurodegeneration in Alzheimer's disease (AD), and both have been associated with microglial activation. However, the specific role of activated microglia in AD pathogenesis remains unresolved. Here we report that microglial cells exhibit significant telomere(definition) shortening and reduction of telomerase activity with normal aging in rats, and that in humans there is a tendency toward telomere shortening with presence of dementia. Human brains containing high amyloid loads demonstrate a significantly higher degree of microglial dystrophy than nondemented, amyloid-free control subjects. Collectively, these findings show that microglial cell senescence(definition) associated with telomere shortening and normal aging is exacerbated by the presence of amyloid. They suggest that degeneration of microglia is a factor in the pathogenesis of AD.

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Provenance

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OpenAlex
DOI
10.1089/rej.2006.9096
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2026-06-22 MST

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APA
Flanary, B., Sammons, N.W., Nguyen, C.T., Walker, D.G., &amp; Streit, W.J. (2007). Evidence That Aging And Amyloid Promote Microglial Cell Senescence. <em>Rejuvenation Research</em>. https://doi.org/10.1089/rej.2006.9096
Vancouver
Flanary B, Sammons NW, Nguyen CT, Walker DG, Streit WJ. Evidence That Aging And Amyloid Promote Microglial Cell Senescence. Rejuvenation Research. 2007. doi:10.1089/rej.2006.9096.
BibTeX
@article{barry2007Eviden, title = {Evidence That Aging And Amyloid Promote Microglial Cell Senescence}, author = {Barry Flanary and Nicole W. Sammons and Cuong Thach Nguyen and Douglas G. Walker and Wolfgang J. Streit}, journal = {Rejuvenation Research}, year = {2007}, doi = {10.1089/rej.2006.9096}, }

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