Unimolecular Chemiexcited Oxygenation of Pathogenic Amyloids

Author:

Umeda Hiroki1,Suda Kayo2,Yokogawa Daisuke2,Azumaya Yuto1,Kitada Nobuo3,Maki Shojiro A.3,Kawashima Shigehiro A.1,Mitsunuma Harunobu1,Yamanashi Yuki1,Kanai Motomu1ORCID

Affiliation:

1. Graduate School of Pharmaceutical Sciences The University of Tokyo Tokyo 113-0033 Japan

2. Graduate School of Arts and Sciences The University of Tokyo Tokyo 153-8902 Japan

3. Graduate School of Informatics and Engineering The University of Electro-Communications, Chofu Tokyo 182-8585 Japan

Abstract

AbstractPathogenic protein aggregates, called amyloids, are etiologically relevant to various diseases, including neurodegenerative Alzheimer disease. Catalytic photooxygenation of amyloids, such as amyloid‐β (Aβ), reduces their toxicity; however, the requirement for light irradiation may limit its utility in large animals, including humans, due to the low tissue permeability of light. Here, we report that Cypridina luciferin analogs, dmCLA‐Cl and dmCLA‐Br, promoted selective oxygenation of amyloids through chemiexcitation without external light irradiation. Further structural optimization of dmCLA‐Cl led to the identification of a derivative with a polar carboxylate functional group and low cellular toxicity: dmCLA‐Cl‐acid. dmCLA‐Cl‐acid promoted oxygenation of Aβ amyloid and reduced its cellular toxicity without photoirradiation. The chemiexcited oxygenation developed in this study may be an effective approach to neutralizing the toxicity of amyloids, which can accumulate deep inside the body, and treating amyloidosis.

Funder

Japan Society for the Promotion of Science

Japan Science and Technology Corporation

Publisher

Wiley

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