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The role of anionic peptide fragments in 1N4R human tau protein aggregation
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نویسنده
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khalili m.a.n. ,riazi g. ,ahmadian s. ,khodarahmi r. ,khodadadi s. ,afrasiabi a. ,karima o. ,mokhtari f. ,hoveizi e.
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منبع
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protein and peptide letters - 2014 - دوره : 21 - شماره : 6 - صفحه:511 -516
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چکیده
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Cellular protein degradation systems are necessary to avoid the accumulation of misfolded or damaged proteins. deficiency in these systems might cause to partial degradation of misfolded proteins and generation of amyloidogenic fragments. protein misfolding is believed to be the primary cause of neurodegenerative disorders such as alzheimer's disease (ad). in this study,we investigate effect of two anionic peptide fragments including,an acidic fragment of human aβ (aβ1-11) and a phosphorylated fragment of β-casein (tetraphosphopeptide),on tau protein aggregation. according to our results,these peptide fragments,induced tau fibrillization in vitro. in sum,we suggest that structural and conformational characters of inducer are as important as charge distribution on anionic inducer molecules however more experiments would be need to exactly confirm this suggestion. © 2014 bentham science publishers.
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کلیدواژه
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Aggregation; Human Aβ1-11; Protein misfolding; Tau; β-Casein Tetraphosphopeptide
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آدرس
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university of tehran, ایران, university of tehran, ایران, university of tehran, ایران, department of pharmacognosy and biotechnology,faculty of pharmacy,kermanshah university of medical sciences, ایران, university of tehran, ایران, university of tehran, ایران, university of tehran, ایران, university of tehran, ایران, department of biology,faculty of sciences,university of tarbiat moallem, ایران
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Authors
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