Development of a New Distyrylbenzene-Derivative Amyloid-β-aggregation and Fibril Formation Inhibitor
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概要
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Several new amyloid-β (Aβ) aggregation inhibitors were synthesized according to our theory that a hydrophilic moiety could be attached to the Aβ-recognition unit for the purpose of preventing amyloid plaque formation. A distyrylbenzene-derivative, DSB(EEX)3, which consider the Aβ recognition unit (DSB, 1,4-distyrylbenzene) and expected to bind to amyloid fibrils (β-sheet structure), was combined with the hydrophilic aggregation disrupting element (EEX) (E, Glu; X, 2-(2-(2-aminoethoxy)ethoxy)acetic acid). This DSB(EEX)3 compound, compared to several others synthesized similarly, was found to be the most active for reducing Aβ toxicity toward IMR-32 human neuroblastoma cells. Moreover, its inhibition of Aβ-aggregation or fibril formation was directly confirmed by transmission electron microscopy and atomic force microscopy. These results suggest that the Aβ aggregation inhibitor DSB(EEX)3 disrupts clumps of Aβ protein and is a likely candidate for drug development to treat Alzheimer’s disease.
著者
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Ishigami Akihito
Molecular Regulation of Aging, Tokyo Metropolitan Institute of Gerontology
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Ishigami Akihito
Molecular Regulation Of Aging Tokyo Metropolitan Inst. Of Gerontology
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Maruyama Naoki
Molecular Regulation Of Aging Research Team For Functional Biogerontology Tokyo Metropolitan Institu
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Handa Setsuko
Molecular Regulation Of Aging Tokyo Metropolitan Institute Of Gerontology
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Suzuki Hideharu
Faculty of Pharmaceutical Sciences, Toho University
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Orimoto Ayako
Faculty of Pharmaceutical Sciences, Toho University
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Matsuyama Akihiro
Faculty of Pharmaceutical Sciences, Toho University
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Yokoyama Yuusaku
Faculty of Pharmaceutical Sciences, Toho University
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Okuno Hiroaki
Faculty of Pharmaceutical Sciences, Toho University
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Nakakoshi Masamichi
Faculty of Pharmaceutical Sciences, Toho University
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