Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils

Jan Bieschke; Martin Herbst; Thomas Wiglenda; Ralf P. Friedrich; Annett Boeddrich; Franziska Schiele; Daniela Kleckers; Juan Miguel Lopez Del Amo; Björn A. Grüning; Qinwen Wang; Michael R. Schmidt; Rudi Lurz; Roger Anwyl; Sigrid Schnoegl; Marcus Fändrich; Ronald F. Frank; Bernd Reif; Stefan Günther; Dominic M. Walsh; Erich E. Wanker

doi:10.1038/nchembio.719

Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils

Jan Bieschke, Martin Herbst, Thomas Wiglenda, Ralf P. Friedrich, Annett Boeddrich, Franziska Schiele, Daniela Kleckers, Juan Miguel Lopez Del Amo, Björn A. Grüning, Qinwen Wang, Michael R. Schmidt, Rudi Lurz, Roger Anwyl, Sigrid Schnoegl, Marcus Fändrich, Ronald F. Frank, Bernd Reif, Stefan Günther, Dominic M. Walsh, Erich E. Wanker

Associate Professorship of Solid-State NMR spectroscopy

Research output: Contribution to journal › Article › peer-review

390 Scopus citations

Abstract

Several lines of evidence indicate that prefibrillar assemblies of amyloid-β (Aβ) polypeptides, such as soluble oligomers or protofibrils, rather than mature, end-stage amyloid fibrils cause neuronal dysfunction and memory impairment in Alzheimer's disease. These findings suggest that reducing the prevalence of transient intermediates by small moleculeg-mediated stimulation of amyloid polymerization might decrease toxicity. Here we demonstrate the acceleration of Aβ fibrillogenesis through the action of the orcein-related small molecule O4, which directly binds to hydrophobic amino acid residues in Aβ peptides and stabilizes the self-assembly of seeding-competent, β-sheetg-rich protofibrils and fibrils. Notably, the O4-mediated acceleration of amyloid fibril formation efficiently decreases the concentration of small, toxic Aβ oligomers in complex, heterogeneous aggregation reactions. In addition, O4 treatment suppresses inhibition of long-term potentiation by Aβ oligomers in hippocampal brain slices. These results support the hypothesis that small, diffusible prefibrillar amyloid species rather than mature fibrillar aggregates are toxic for mammalian cells.

Original language	English
Pages (from-to)	93-101
Number of pages	9
Journal	Nature Chemical Biology
Volume	8
Issue number	1
DOIs	https://doi.org/10.1038/nchembio.719
State	Published - Jan 2012

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Bieschke, J., Herbst, M., Wiglenda, T., Friedrich, R. P., Boeddrich, A., Schiele, F., Kleckers, D., Lopez Del Amo, J. M., Grüning, B. A., Wang, Q., Schmidt, M. R., Lurz, R., Anwyl, R., Schnoegl, S., Fändrich, M., Frank, R. F., Reif, B., Günther, S., Walsh, D. M., & Wanker, E. E. (2012). Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils. Nature Chemical Biology, 8(1), 93-101. https://doi.org/10.1038/nchembio.719

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title = "Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils",

abstract = "Several lines of evidence indicate that prefibrillar assemblies of amyloid-β (Aβ) polypeptides, such as soluble oligomers or protofibrils, rather than mature, end-stage amyloid fibrils cause neuronal dysfunction and memory impairment in Alzheimer's disease. These findings suggest that reducing the prevalence of transient intermediates by small moleculeg-mediated stimulation of amyloid polymerization might decrease toxicity. Here we demonstrate the acceleration of Aβ fibrillogenesis through the action of the orcein-related small molecule O4, which directly binds to hydrophobic amino acid residues in Aβ peptides and stabilizes the self-assembly of seeding-competent, β-sheetg-rich protofibrils and fibrils. Notably, the O4-mediated acceleration of amyloid fibril formation efficiently decreases the concentration of small, toxic Aβ oligomers in complex, heterogeneous aggregation reactions. In addition, O4 treatment suppresses inhibition of long-term potentiation by Aβ oligomers in hippocampal brain slices. These results support the hypothesis that small, diffusible prefibrillar amyloid species rather than mature fibrillar aggregates are toxic for mammalian cells.",

author = "Jan Bieschke and Martin Herbst and Thomas Wiglenda and Friedrich, {Ralf P.} and Annett Boeddrich and Franziska Schiele and Daniela Kleckers and {Lopez Del Amo}, {Juan Miguel} and Gr{\"u}ning, {Bj{\"o}rn A.} and Qinwen Wang and Schmidt, {Michael R.} and Rudi Lurz and Roger Anwyl and Sigrid Schnoegl and Marcus F{\"a}ndrich and Frank, {Ronald F.} and Bernd Reif and Stefan G{\"u}nther and Walsh, {Dominic M.} and Wanker, {Erich E.}",

year = "2012",

month = jan,

doi = "10.1038/nchembio.719",

language = "English",

volume = "8",

pages = "93--101",

journal = "Nature Chemical Biology",

issn = "1552-4450",

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Bieschke, J, Herbst, M, Wiglenda, T, Friedrich, RP, Boeddrich, A, Schiele, F, Kleckers, D, Lopez Del Amo, JM, Grüning, BA, Wang, Q, Schmidt, MR, Lurz, R, Anwyl, R, Schnoegl, S, Fändrich, M, Frank, RF, Reif, B, Günther, S, Walsh, DM & Wanker, EE 2012, 'Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils', Nature Chemical Biology, vol. 8, no. 1, pp. 93-101. https://doi.org/10.1038/nchembio.719

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AU - Herbst, Martin

AU - Wiglenda, Thomas

AU - Friedrich, Ralf P.

AU - Boeddrich, Annett

AU - Schiele, Franziska

AU - Kleckers, Daniela

AU - Lopez Del Amo, Juan Miguel

AU - Grüning, Björn A.

AU - Wang, Qinwen

AU - Schmidt, Michael R.

AU - Lurz, Rudi

AU - Anwyl, Roger

AU - Schnoegl, Sigrid

AU - Fändrich, Marcus

AU - Frank, Ronald F.

AU - Reif, Bernd

AU - Günther, Stefan

AU - Walsh, Dominic M.

AU - Wanker, Erich E.

PY - 2012/1

Y1 - 2012/1

N2 - Several lines of evidence indicate that prefibrillar assemblies of amyloid-β (Aβ) polypeptides, such as soluble oligomers or protofibrils, rather than mature, end-stage amyloid fibrils cause neuronal dysfunction and memory impairment in Alzheimer's disease. These findings suggest that reducing the prevalence of transient intermediates by small moleculeg-mediated stimulation of amyloid polymerization might decrease toxicity. Here we demonstrate the acceleration of Aβ fibrillogenesis through the action of the orcein-related small molecule O4, which directly binds to hydrophobic amino acid residues in Aβ peptides and stabilizes the self-assembly of seeding-competent, β-sheetg-rich protofibrils and fibrils. Notably, the O4-mediated acceleration of amyloid fibril formation efficiently decreases the concentration of small, toxic Aβ oligomers in complex, heterogeneous aggregation reactions. In addition, O4 treatment suppresses inhibition of long-term potentiation by Aβ oligomers in hippocampal brain slices. These results support the hypothesis that small, diffusible prefibrillar amyloid species rather than mature fibrillar aggregates are toxic for mammalian cells.

AB - Several lines of evidence indicate that prefibrillar assemblies of amyloid-β (Aβ) polypeptides, such as soluble oligomers or protofibrils, rather than mature, end-stage amyloid fibrils cause neuronal dysfunction and memory impairment in Alzheimer's disease. These findings suggest that reducing the prevalence of transient intermediates by small moleculeg-mediated stimulation of amyloid polymerization might decrease toxicity. Here we demonstrate the acceleration of Aβ fibrillogenesis through the action of the orcein-related small molecule O4, which directly binds to hydrophobic amino acid residues in Aβ peptides and stabilizes the self-assembly of seeding-competent, β-sheetg-rich protofibrils and fibrils. Notably, the O4-mediated acceleration of amyloid fibril formation efficiently decreases the concentration of small, toxic Aβ oligomers in complex, heterogeneous aggregation reactions. In addition, O4 treatment suppresses inhibition of long-term potentiation by Aβ oligomers in hippocampal brain slices. These results support the hypothesis that small, diffusible prefibrillar amyloid species rather than mature fibrillar aggregates are toxic for mammalian cells.

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Small-molecule conversion of toxic oligomers to nontoxic β-sheetg-rich amyloid fibrils

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