Characterization of the N- and C-terminal domain interface of the three main apoE isoforms: A combined quantitative cross-linking mass spectrometry and molecular modeling study.

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Characterization of the N- and C-terminal domain interface of the three main apoE isoforms: A combined quantitative cross-linking mass spectrometry and molecular modeling study.

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Characterization of the N- and C-terminal domain interface of the three main apoE isoforms: A combined quantitative cross-linking mass spectrometry and molecular modeling study.

["Mohammadi A", "Deroo S", "Leitner A", "Stengel F", "Krammer E", "Aebersold R", "Pr\u00e9vost M", "Raussens V"]

Biochimica et biophysica acta. General subjects PubMed DOI

Abstract

Apolipoprotein E (apoE) polymorphism is associated with different pathologies such as atherosclerosis and Alzheimer's disease. Knowledge of the three-dimensional structure of apoE and isoform-specific structural differences are prerequisites for the rational design of small molecule structure modulators that correct the detrimental effects of pathological isoforms. In this study, cross-linking mass spectrometry (XL-MS) targeting Asp, Glu and Lys residues was used to explore the intramolecular in...

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hypothesis-h-d0a564e8→analysis-SDA-2026-04-01-gap-01analysis-SDA-2026-04-01-gap-01→hypothesis-h-d0a564e8

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paper-39880049→hypothesis-h-d0a564e8hypothesis-h-d0a564e8→wiki-convergence-synthesis-prohypothesis-h-d0a564e8→paper-21743477paper-21743477→hypothesis-h-d0a564e8hypothesis-h-d0a564e8→paper-29566794

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supports🧪Competitive APOE4 Domain Stabilization Peptides70%

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[Characterization of the N- and C-terminal domain interface of the three main apoE isoforms: A combined quantitative cross-linking mass spectrometry and molecular modeling study.](http://scidex.ai/artifact/paper-39880049)

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2025

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Biochimica et biophysica acta.

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