Article ID Journal Published Year Pages File Type
1949450 Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biology of Lipids 2012 8 Pages PDF
Abstract

The association between apolipoprotein E (apoE) and amyloid-β peptide (Aβ) may significantly impact the function of both proteins, thus affecting the etiology of Alzheimer's disease (AD). However, apoE/Aβ interactions remain fundamentally defined by the stringency of the detection method. Here we use size exclusion chromatography (SEC) as a non-stringent approach to the detection of apoE/Aβ interactions in solution, specifically apoE and both endogenous and exogenous Aβ from plasma, CSF and astrocyte conditioned media. By SEC analysis, Aβ association with plasma and CNS lipoproteins is apoE-dependent. While endogenous Aβ elutes to specific human plasma lipoproteins distinct from those containing apoE, it is the apoE-containing lipoproteins that absorb excess amounts of exogenous Aβ40. In human CSF, apoE, endogenous Aβ and phospholipid elute in an almost identical profile, as do apoE, exogenous Aβ and phospholipid from astrocyte conditioned media. Combining SEC fractionation with subsequent analysis for SDS-stable apoE/Aβ complex reveals that apoE-containing astrocyte lipoproteins exhibit the most robust interactions with Aβ. Thus, standardization of the methods for detecting apoE/Aβ complex is necessary to determine its functional significance in the neuropathology characteristic of AD. Importantly, a systematic understanding of the role of apoE-containing plasma and CNS lipoproteins in Aβ homeostasis could potentially contribute to identifying a plasma biomarker currently over-looked because it has multiple components.

► SEC is a non-stringent approach to the detection of apoE/Aβ interactions in solution. ► By SEC analysis, Aβ association with CNS and plasma lipoproteins is apoE-dependent. ► ApoE-containing human plasma lipoproteins absorb excess amounts of exogenous Aβ40. ► Aβ and apoE-containing astrocyte lipoproteins exhibit the most robust interaction. ► Aβ/lipoprotein interactions are important for clearance and as a potential biomarker.

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Life Sciences Biochemistry, Genetics and Molecular Biology Biochemistry
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