Molecular basis underlying the specificity of an antagonist AA92593 for mammalian melanopsins

Obayashi, Kohei; Zou, Ruisi; Kawaguchi, Tomoki; Mori, Toshifumi; Tsukamoto, Hisao

https://hdl.handle.net/20.500.14094/0100495833

このアイテムのアクセス数:45件（2025-07-02 14:47 集計）

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メタデータID	0100495833
アクセス権	open access
出版タイプ	Version of Record
タイトル	Molecular basis underlying the specificity of an antagonist AA92593 for mammalian melanopsins
著者	Obayashi, Kohei ; Zou, Ruisi ; Kawaguchi, Tomoki ; Mori, Toshifumi ; Tsukamoto, Hisao
著者名 Obayashi, Kohei
著者名 Zou, Ruisi
著者名 Kawaguchi, Tomoki
著者名 Mori, Toshifumi
著者ID A2635 研究者ID 1000090579814 KUID https://kuid-rm-web.ofc.kobe-u.ac.jp/search/detail.html?systemId=b5431fc98a1dc7bc520e17560c007669 著者名 Tsukamoto, Hisao 塚本, 寿夫ツカモト, ヒサオ所属機関名理学研究科
言語	English (英語)
収録物名	Journal of Biological Chemistry
巻(号)	301(5)
ページ	108461
出版者	Elsevier
刊行日	2025-05
公開日	2025-05-12
抄録	Melanopsin functions in intrinsically photosensitive retinal ganglion cells of mammals to regulate circadian clock and pupil constriction. The opsinamide AA92593 has been reported to specifically inhibit mouse and human melanopsin functions as a competitive antagonist against retinal; however, the molecular mechanisms underlying its specificity have not been resolved. In this study, we attempted to identify amino acid residues responsible for the susceptibility of mammalian melanopsins to AA92593. Our cell-based assays confirmed that AA92593 effectively inhibited the light-induced cellular responses of mammalian melanopsins, but not those of non-mammalian vertebrate and invertebrate melanopsins. These results suggest that amino acid residues specifically conserved among mammalian melanopsins are important for the antagonistic effect of AA92593, and we noticed Phe-94².⁶¹, Ser-188ᴱᶜᴸ², and Ser-269⁶.⁵² as candidate residues. Substitutions of these residues reduced the antagonistic effect of AA92593. We conducted docking and molecular dynamics simulations based on the AlphaFold-predicted melanopsin structure. The simulations indicated that Phe-94².⁶¹, Ser-188ᴱᶜᴸ², and Ser-269⁶.⁵² are located at the AA92593-binding site and additionally identified Trp-189ᴱᶜᴸ² and Leu-207⁵.⁴² interacting with the antagonist. Substitutions of Trp-189ᴱᶜᴸ² and Leu-207⁵.⁴² affected the antagonistic effect of AA92593. Furthermore, substitutions of these amino acid residues converted the AA92593-insensitive non-mammalian melanopsins susceptible to the antagonist. Based on experiments and molecular simulations, five amino acid residues, at positions 94².⁶¹, 188ᴱᶜᴸ², 189ᴱᶜᴸ², 207⁵.⁴², and 269⁶.⁵², were found to be responsible for the specific susceptibility of mammalian melanopsins to AA92593.
キーワード	melanopsin
	opsin
	GPCR
	antagonist
	molecular dynamics
	non-visual photoreception
カテゴリ	理学研究科
カテゴリ	学術雑誌論文
権利	© 2025 The Authors. Published by Elsevier Inc on behalf of American Society for Biochemistry and Molecular Biologyé
権利	This is an open access article under the Creative Commons Attribution 4.0 International license
関連情報	DOI https://doi.org/10.1016/j.jbc.2025.108461
関連情報	PMID 40154611

資源タイプ	journal article
ISSN	0021-9258　OPACで所蔵を検索　 CiNiiで学外所蔵を検索
eISSN	1083-351X　OPACで所蔵を検索　 CiNiiで学外所蔵を検索

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