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| Type |
Poster Presentation |
| Area |
Inorganic Chemistry |
| Room No. |
Exhibition Hall 2+3 |
| Time |
10월 19일 (목요일) 11:00~12:30 |
| Code |
INOR.P-11 |
| Subject |
Strategic Design of 2,2’-Bipyridine Derivatives to Modulate Metal-Amyloid-β Aggregation
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| Authors |
Yongwhan Ji, Hyuck Jin Lee1, Jaeheung Cho2, Cheol Min Park*, Mi Hee Lim*
Department of Chemistry, Ulsan National Institute of Science and Technology, Korea
1Department of Life Science, Ulsan National Institute of Science and Technology, Korea
2Emerging Materials Science, Daegu Gyeongbuk Institute of Science & Technology, Korea
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| Abstract |
The complexity of Alzheimer’s disease (AD) stems from the inter-relation of multiple pathological factors upon initiation and progression of the disease. To identify the involvement of metal–bound amyloid-β (metal-Aβ) aggregation in AD pathology, among the pathogenic features found in the AD-affected brain, small molecules as chemical tools capable of controlling metal-Aβ aggregation were developed. Herein, we report a new class of 2,2’-bipyridine (bpy) derivatives (1–4) rationally designed to be chemical modulators toward metal-Aβ aggregation over metal-free Aβ analogue. The bpy derivatives were constructed through a rational design strategy employing straightforward structural variations onto the backbone of a metal chelator, bpy: (i) incorporation of an Aβ interacting moiety; (ii) introduction of a methyl group at different positions. The newly prepared bpy derivatives were observed to bind to metal ions [i.e., Cu(II) and Zn(II)] and interact with metal–Aβ over metal-free Aβ to varying degrees. Distinguishable from bpy, the bpy derivatives (1–3) were indicated to noticeably modulate the aggregation pathways of Cu(II)–Aβ and Zn(II)–Aβ over metal-free Aβ. Overall, our studies of the bpy derivatives demonstrate that the alteration of metal binding properties as well as the installation of an Aβ interacting capability onto a metal chelating framework, devised via the rational structure-based design, were able to achieve evident modulating reactivity against metal–Aβ aggregation. Obviating the need for complicated structures, our design approach, presented in this work, could be appropriately utilized for inventing small molecules as chemical tools for studying desired metal-related targets in biological systems. |
| E-mail |
op9595@unist.ac.kr |
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120th General Meeting of the KCS