Leuco Ethyl Violet as Self‐Activating Prodrug Photocatalyst for In Vivo Amyloid‐Selective Oxygenation

Author:

Furuta Masahiro1,Arii Suguru1,Umeda Hiroki1,Matsukawa Ryota1,Shizu Katsuyuki2,Kaji Hironori2,Kawashima Shigehiro A.1,Hori Yukiko1,Tomita Taisuke1,Sohma Youhei3,Mitsunuma Harunobu14,Kanai Motomu1ORCID

Affiliation:

1. Graduate School of Pharmaceutical Sciences The University of Tokyo 7‐3‐1 Hongo, Bunkyo‐ku Tokyo 113‐0033 Japan

2. Institute for Chemical Research Kyoto University Kyoto 611‐0011 Japan

3. School of Pharmaceutical Sciences Wakayama Medical University Wakayama 640‐8156 Japan

4. PRESTO JST 4‐1‐8 Honcho, Kawaguchi Saitama 332‐0012 Japan

Abstract

AbstractAberrant aggregates of amyloid‐β (Aβ) and tau protein (tau), called amyloid, are related to the etiology of Alzheimer disease (AD). Reducing amyloid levels in AD patients is a potentially effective approach to the treatment of AD. The selective degradation of amyloids via small molecule‐catalyzed photooxygenation in vivo is a leading approach; however, moderate catalyst activity and the side effects of scalp injury are problematic in prior studies using AD model mice. Here, leuco ethyl violet (LEV) is identified as a highly active, amyloid‐selective, and blood‐brain barrier (BBB)‐permeable photooxygenation catalyst that circumvents all of these problems. LEV is a redox‐sensitive, self‐activating prodrug catalyst; self‐oxidation of LEV through a hydrogen atom transfer process under photoirradiation produces catalytically active ethyl violet (EV) in the presence of amyloid. LEV effectively oxygenates human Aβ and tau, suggesting the feasibility for applications in humans. Furthermore, a concept of using a hydrogen atom as a caging group of a reactive catalyst functional in vivo is postulated. The minimal size of the hydrogen caging group is especially useful for catalyst delivery to the brain through BBB.

Funder

Japan Science and Technology Corporation

Japan Society for the Promotion of Science

Publisher

Wiley

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