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- Live5/17/2026, 4:45:12 PM
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{ "field_tag": "astrocytes", "text": "What resolves this contention: APOE4 drives AD pathology through gain-of-toxic-function: early apoE4 overexpression strongly increases plaque load, apoE4 particles are abnormally large, and APOE4 has broad detrimental effects on tau, microglia, and astrocyte reactivity beyond amyloid-β vs. APOE4 effects may partly reflect loss-of-function: apoE4 has reduced half-life, constitutes only 30–40% of total apoE in heterozygous mice, and ASO-mediated APOE suppression reduces plaques, suggesting reducing apoE (including apoE4) is beneficial / APOE ε4 allele remains the strongest genetic risk factor for sporadic Alzheimer's disease, with pathogenic mechanisms now understood to extend beyond amyloid-β to include tau neurodegeneration, microglia and astrocyte responses, and blood-brain barrier disruption. / In targeted replacement APOE3/4 mice, apoE4 constitutes only 30–40% of total apoE levels due to enhanced degradation and re", "source_refs": [ "paper:paper-c05fea99dd6f", "paper:paper-d74c3cfc15b9", "wiki_page:computationalreviewastrocytes-12", "paper:paper-c05fea99dd6f", "paper:paper-d74c3cfc15b9", "wiki_page:computationalreviewastrocytes-12", "paper:paper-c05fea99dd6f", "paper:paper-d74c3cfc15b9", "wiki_page:computationalreviewastrocytes-12", "paper:paper-c05fea99dd6f", "paper:paper-d74c3cfc15b9", "wiki_page:computationalreviewastrocytes-12" ], "importance": "0.7200", "tractability": "0.5500", "potential_impact": "0.7000", "composite_score": "0.2772", "elo_rating": "1500.00", "state": "open", "decay_rate": "0.01000", "resolution_evidence_refs": [] }