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• W4379536640 abstract "Abstract Background Apolipoprotein E (ApoE) ε4 genotype is the most prevalent risk factor for late-onset Alzheimer’s Disease (AD). Although ApoE4 differs from its non-pathological ApoE3 isoform only by the C112R mutation, the molecular mechanism of its proteinopathy is unknown. Methods Here, we reveal the molecular mechanism of ApoE4 aggregation using a combination of experimental and computational techniques, including X-ray crystallography, site-directed mutagenesis, hydrogen-deuterium mass spectrometry (HDX-MS), static light scattering and molecular dynamics simulations. Treatment of ApoE ε3/ε3 and ε4/ε4 cerebral organoids with tramiprosate was used to compare the effect of tramiprosate on ApoE4 aggregation at the cellular level. Results We found that C112R substitution in ApoE4 induces long-distance (> 15 Å) conformational changes leading to the formation of a V-shaped dimeric unit that is geometrically different and more aggregation-prone than the ApoE3 structure. AD drug candidate tramiprosate and its metabolite 3-sulfopropanoic acid induce ApoE3-like conformational behavior in ApoE4 and reduce its aggregation propensity. Analysis of ApoE ε4/ε4 cerebral organoids treated with tramiprosate revealed its effect on cholesteryl esters, the storage products of excess cholesterol. Conclusions Our results connect the ApoE4 structure with its aggregation propensity, providing a new druggable target for neurodegeneration and ageing. Graphic Abstract" @default.
• W4379536640 created "2023-06-07" @default.
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• W4379536640 date "2023-06-06" @default.
• W4379536640 modified "2023-10-17" @default.
• W4379536640 title "Domino-like effect of C112R mutation on ApoE4 aggregation and its reduction by Alzheimer’s Disease drug candidate" @default.
• W4379536640 cites W1031578623 @default.
• W4379536640 cites W1546262989 @default.
• W4379536640 cites W1559121591 @default.
• W4379536640 cites W1559890486 @default.
• W4379536640 cites W1573009101 @default.
• W4379536640 cites W1968984443 @default.
• W4379536640 cites W1969189143 @default.
• W4379536640 cites W1975317507 @default.
• W4379536640 cites W1976499671 @default.
• W4379536640 cites W1989076425 @default.
• W4379536640 cites W1990016625 @default.
• W4379536640 cites W1991166529 @default.
• W4379536640 cites W1994778680 @default.
• W4379536640 cites W2002181764 @default.
• W4379536640 cites W2006599070 @default.
• W4379536640 cites W2008708467 @default.
• W4379536640 cites W2014055987 @default.
• W4379536640 cites W2028046413 @default.
• W4379536640 cites W2030971064 @default.
• W4379536640 cites W2032061707 @default.
• W4379536640 cites W2035467780 @default.
• W4379536640 cites W2036362108 @default.
• W4379536640 cites W2041791898 @default.
• W4379536640 cites W2056451248 @default.
• W4379536640 cites W2059995793 @default.
• W4379536640 cites W2061950854 @default.
• W4379536640 cites W2066768773 @default.
• W4379536640 cites W2067160010 @default.
• W4379536640 cites W2067976699 @default.
• W4379536640 cites W2069118296 @default.
• W4379536640 cites W2072321657 @default.
• W4379536640 cites W2072682191 @default.
• W4379536640 cites W2076775566 @default.
• W4379536640 cites W2076790509 @default.
• W4379536640 cites W2079793886 @default.
• W4379536640 cites W2082586732 @default.
• W4379536640 cites W2082846873 @default.
• W4379536640 cites W2084692275 @default.
• W4379536640 cites W2087532566 @default.
• W4379536640 cites W2089657004 @default.
• W4379536640 cites W2090688839 @default.
• W4379536640 cites W2090966154 @default.
• W4379536640 cites W2091701505 @default.
• W4379536640 cites W2095719702 @default.
• W4379536640 cites W2097149810 @default.
• W4379536640 cites W2103139149 @default.
• W4379536640 cites W2105103540 @default.
• W4379536640 cites W2109180944 @default.
• W4379536640 cites W2109910226 @default.
• W4379536640 cites W2110808180 @default.
• W4379536640 cites W2111135465 @default.
• W4379536640 cites W2116439437 @default.
• W4379536640 cites W2119556701 @default.
• W4379536640 cites W2124026197 @default.
• W4379536640 cites W2128824543 @default.
• W4379536640 cites W2140205792 @default.
• W4379536640 cites W2161925307 @default.
• W4379536640 cites W2163341755 @default.
• W4379536640 cites W2165557965 @default.
• W4379536640 cites W2168708922 @default.
• W4379536640 cites W2296686360 @default.
• W4379536640 cites W2332712348 @default.
• W4379536640 cites W2410593854 @default.
• W4379536640 cites W2471406522 @default.
• W4379536640 cites W2471981404 @default.
• W4379536640 cites W2555870966 @default.
• W4379536640 cites W2564454435 @default.
• W4379536640 cites W2574219503 @default.
• W4379536640 cites W2606668492 @default.
• W4379536640 cites W2618913695 @default.
• W4379536640 cites W2765415508 @default.
• W4379536640 cites W2774482055 @default.

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