2021
DOI: 10.1016/j.bpc.2020.106505
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Visualizing and trapping transient oligomers in amyloid assembly pathways

Abstract: Oligomers which form during amyloid fibril assembly are considered to be key contributors towards amyloid disease. However, understanding how such intermediates form, their structure, and mechanisms of toxicity presents significant challenges due to their transient and heterogeneous nature. Here, we discuss two different strategies for addressing these challenges: use of (1) methods capable of detecting lowly-populated species within complex mixtures, such as NMR, single particle methods (including fluorescenc… Show more

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Cited by 110 publications
(94 citation statements)
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References 261 publications
(367 reference statements)
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“…Here, we use liquid-state NMR spectroscopy ( 30 , 31 ) to show that EGCG binds to monomeric and oligomeric αSN. We find that monomeric and oligomeric αSN bind 54 and 7 EGCG molecules, respectively, and that EGCG slowly (over a 4-day period) binds to and immobilizes all protein residues.…”
mentioning
confidence: 99%
“…Here, we use liquid-state NMR spectroscopy ( 30 , 31 ) to show that EGCG binds to monomeric and oligomeric αSN. We find that monomeric and oligomeric αSN bind 54 and 7 EGCG molecules, respectively, and that EGCG slowly (over a 4-day period) binds to and immobilizes all protein residues.…”
mentioning
confidence: 99%
“…Amyloid aggregation is a critical step in neurodegenerative disease and recent emphasis on oligomeric intermediates in this process as disease active agents has triggered the search for novel methods to measure such intermediates, see for example [1,2]. Alpha-synuclein (αS) is an interesting example, as it is a functional protein in the brain, where it is suggested to be involved in neuronal-vesicle fusion to the synapse, and thereby important in the neurotransmitter release in the synapse [3,4].…”
Section: Introductionmentioning
confidence: 99%
“…[2][3][4] Amyloid formation of Aβ is typically viewed as a nucleated polymerization process, manifested by an initial lag phase in which the oligomeric nuclei are formed, followed by a rapid growth phase during which the nuclei grow by the addition of monomers to form fibrillar structures. [5][6] Moreover, amyloid oligomers has also shown to form hetero-oligomers by interacting with its isoforms or other proteins. 5,7 Therefore great effort have been devoted to characterized oligomers to better understand amyloid mechanism and conceived plausible therapeutics alternatives.…”
Section: Introductionmentioning
confidence: 99%
“…5,7 Therefore great effort have been devoted to characterized oligomers to better understand amyloid mechanism and conceived plausible therapeutics alternatives. 4,6 One of the plausible therapeutic strategies for treating the disease is to inhibit the formation of toxic Aβ aggregate species. As such, a wide variety of amyloid inhibitors that can prevent the formation of Aβ aggregates, e.g., small organic compounds and designed peptides, have been reported.…”
Section: Introductionmentioning
confidence: 99%