Massive gliosis induced by interleukin‐6 suppresses Aβ deposition in vivo: evidence against inflammation as a driving force for amyloid deposition

Massive gliosis induced by interleukin‐6 suppresses Aβ deposition in vivo: evidence against inflammation as a driving force for amyloid deposition

Proinflammatory stimuli, after amyloid β (Aβ) deposition, have been hypothesized to create a self‐reinforcing positive feedback loop that increases amyloidogenic processing of the Aβ precursor protein (APP), promoting further Aβ accumulation and neuroinflammation in Alzheimer's disease (AD). In...

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Veröffentlicht in:The FASEB journal 2010-02, Vol.24 (2), p.548-559
Hauptverfasser: Chakrabarty, Paramita, Jansen‐West, Karen, Beccard, Amanda, Ceballos‐Diaz, Carolina, Levites, Yona, Verbeeck, Christophe, Zubair, Abba C., Dickson, Dennis, Golde, Todd E., Das, Pritam
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Alzheimer's disease
APP
neuroinflammation
recombinant adeno‐associated virus
Research Communications
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container_end_page 559
container_issue 2
container_start_page 548
container_title The FASEB journal
container_volume 24
creator Chakrabarty, Paramita
Jansen‐West, Karen
Beccard, Amanda
Ceballos‐Diaz, Carolina
Levites, Yona
Verbeeck, Christophe
Zubair, Abba C.
Dickson, Dennis
Golde, Todd E.
Das, Pritam
description Proinflammatory stimuli, after amyloid β (Aβ) deposition, have been hypothesized to create a self‐reinforcing positive feedback loop that increases amyloidogenic processing of the Aβ precursor protein (APP), promoting further Aβ accumulation and neuroinflammation in Alzheimer's disease (AD). Interleukin‐6 (IL‐6), a proinflammatory cytokine, has been shown to be increased in AD patients implying a pathological interaction. To assess the effects of IL‐6 on Aβ deposition and APP processing in vivo,we overexpressed murine IL‐6 (mIL‐6) in the brains of APP transgenic TgCRND8 and TG2576 mice. mIL‐6 expression resulted in extensive gliosis and concurrently attenuated Aβ deposition in TgCRND8 mouse brains. This was accompanied by up‐regulation of glial phagocytic markers in vivo and resulted in enhanced microglia‐mediated phagocytosis of Aβ aggregates in vitro. Further, mIL‐6‐induced neuroinflammation had no effect on APP processing in TgCRND8 and had no effect on APP processing or steady‐state levels of Aβ in young Tg2576 mice. These results indicate that mIL‐6‐mediated reactive gliosis may be beneficial early in the disease process by potentially enhancing Aβ plaque clearance rather than mediating a neurotoxic feedback loop that exacerbates amyloid pathology. This is the first study that methodically dissects the contribution of mIL‐6 with regard to its potential role in modulating Aβ deposition in vivo.—Chakrabarty, P., Jansen‐West, K., Beccard, A., Ceballos‐Diaz, C., Levites, Y., Verbeeck, C., Zubair, A. C., Dickson, D., Golde, T. E., Das, P. Massive gliosis induced by interleukin‐6 suppresses Aβ deposition in vivo: evidence against inflammation as a driving force for amyloid deposition. FASEB J. 24, 548–559 (2010). www.fasebj.org
doi_str_mv 10.1096/fj.09-141754
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source Wiley Journals; Alma/SFX Local Collection
subjects Alzheimer's disease
APP
neuroinflammation
recombinant adeno‐associated virus
Research Communications
title Massive gliosis induced by interleukin‐6 suppresses Aβ deposition in vivo: evidence against inflammation as a driving force for amyloid deposition
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