Apolipoprotein E promotes astrocyte colocalization and degradation of deposited amyloid-β peptides
Author: ["Milla Koistinaho","Suizhen Lin","Xin Wu","Michail Esterman","Deanna Koger","Jeffrey Hanson","Richard Higgs","Feng Liu","Seema Malkani","Kelly R Bales","Steven M Paul"]
Publication: Nature Medicine
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Abstract
We have previously shown that apolipoprotein E (Apoe) promotes the formation of amyloid in brain and that astrocyte-specific expression of APOE markedly affects the deposition of amyloid-β peptides (Aβ) in a mouse model of Alzheimer disease. Given the capacity of astrocytes to degrade Aβ, we investigated the potential role of Apoe in this astrocyte-mediated degradation. In contrast to cultured adult wild-type mouse astrocytes, adult Apoe−/− astrocytes do not degrade Aβ present in Aβ plaque–bearing brain sections in vitro. Coincubation with antibodies to either Apoe or Aβ, or with RAP, an antagonist of the low-density lipoprotein receptor family, effectively blocks Aβ degradation by astrocytes. Phase-contrast and confocal microscopy show that Apoe−/− astrocytes do not respond to or internalize Aβ deposits to the same extent as do wild-type astrocytes. Thus, Apoe seems to be important in the degradation and clearance of deposited Aβ species by astrocytes, a process that may be impaired in Alzheimer disease.
Cite this article
Koistinaho, M., Lin, S., Wu, X. et al. Apolipoprotein E promotes astrocyte colocalization and degradation of deposited amyloid-β peptides. Nat Med 10, 719–726 (2004). https://doi.org/10.1038/nm1058
