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Immobilized Amyloid Hexamer Fragments to Map Active Sites of Amyloid-Targeting Chemicals

Authors
 Cho, Illhwan  ;  Yoon, Soljee  ;  Park, Sunghyun  ;  Hong, Seung Woo  ;  Cho, Eunjung  ;  Kim, Eo su  ;  Kim, Hye Yun  ;  Kim, YoungSoo 
Citation
 ACS Chemical Neuroscience, Vol.14(1) : 9-18, 2023-01 
Journal Title
ACS CHEMICAL NEUROSCIENCE
ISSN
 1948-7193 
Issue Date
2023-01
Keywords
amyloid-? ; peptide synthesis ; fluorescent imaging agents ; aggregation inhibitors ; aggregate dissociators ; mapping assay
Abstract
As amyloid-beta (A beta) peptide is considered a biomarker and pathological culprit of Alzheimer's disease, A beta- targeting compounds have been investigated for diagnostics development and drug discovery of the disorder. Unlike amyloid plaque targeting agents, such as clinically available amyloid radiotracers intercalating into the beta-sheet structures of the aggregates, monomer and oligomer targeting chemicals are difficult to develop, as the transient and polymorphic nature of these peptides impedes their structural understanding. Here, we report a mapping approach to explore targeting residues of A beta-imaging probes and A beta-regulating drug candidates by utilizing a set of fragmented A beta hexamers immobilized on a 96-well microplate in combination with fluorescent full-length A beta for on-plate aggregation. To evaluate the mapping potential of the peptide plate, we tested previously reported fluorescent imaging agents (CRANAD-28, bis-ANS), aggregation inhibitors (curcumin, scyllo-inositol), and aggregate dissociators (necrostatin-1, sunitinib) targeting A beta. Our approach enabled mechanistic understanding of compounds targeting nonfibrillar A beta on an interacting sequence level.
DOI
10.1021/acschemneuro.2c00449
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Psychiatry (정신과학교실) > 1. Journal Papers
Yonsei Authors
Kim, Eosu(김어수) ORCID logo https://orcid.org/0000-0001-9472-9465
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/193651
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