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Redox-active chemical chaperones exhibiting promiscuous binding promote oxidative protein folding under condensed sub-millimolar conditions.
Suzuki, Koki; Nojiri, Ryoya; Matsusaki, Motonori; Mabuchi, Takuya; Kanemura, Shingo; Ishii, Kotone; Kumeta, Hiroyuki; Okumura, Masaki; Saio, Tomohide; Muraoka, Takahiro.
Afiliação
  • Suzuki K; Department of Applied Chemistry, Graduate School of Engineering, Tokyo University of Agriculture and Technology Koganei Tokyo 184-8588 Japan muraoka@go.tuat.ac.jp.
  • Nojiri R; Department of Applied Chemistry, Graduate School of Engineering, Tokyo University of Agriculture and Technology Koganei Tokyo 184-8588 Japan muraoka@go.tuat.ac.jp.
  • Matsusaki M; Division of Molecular Life Science, Institute of Advanced Medical Sciences, Tokushima University Tokushima 770-8503 Japan saio@tokushima-u.ac.jp.
  • Mabuchi T; Frontier Research Institute for Interdisciplinary Sciences, Tohoku University Sendai Miyagi 980-8578 Japan okmasaki@tohoku.ac.jp.
  • Kanemura S; Institute of Fluid Science, Tohoku University Sendai Miyagi 980-8577 Japan.
  • Ishii K; Frontier Research Institute for Interdisciplinary Sciences, Tohoku University Sendai Miyagi 980-8578 Japan okmasaki@tohoku.ac.jp.
  • Kumeta H; Frontier Research Institute for Interdisciplinary Sciences, Tohoku University Sendai Miyagi 980-8578 Japan okmasaki@tohoku.ac.jp.
  • Okumura M; Faculty of Advanced Life Science, Hokkaido University Sapporo Hokkaido 060-0810 Japan.
  • Saio T; Frontier Research Institute for Interdisciplinary Sciences, Tohoku University Sendai Miyagi 980-8578 Japan okmasaki@tohoku.ac.jp.
  • Muraoka T; Division of Molecular Life Science, Institute of Advanced Medical Sciences, Tokushima University Tokushima 770-8503 Japan saio@tokushima-u.ac.jp.
Chem Sci ; 15(32): 12676-12685, 2024 Aug 14.
Article em En | MEDLINE | ID: mdl-39148798
ABSTRACT
Proteins form native structures through folding processes, many of which proceed through intramolecular hydrophobic effect, hydrogen bond and disulfide-bond formation. In vivo, protein aggregation is prevented even in the highly condensed milieu of a cell through folding mediated by molecular chaperones and oxidative enzymes. Chemical approaches to date have not replicated such exquisite mediation. Oxidoreductases efficiently promote folding by the cooperative effects of oxidative reactivity for disulfide-bond formation in the client unfolded protein and chaperone activity to mitigate aggregation. Conventional synthetic folding promotors mimic the redox-reactivity of thiol/disulfide units but do not address client-recognition units for inhibiting aggregation. Herein, we report thiol/disulfide compounds containing client-recognition units, which act as synthetic oxidoreductase-mimics. For example, compound ßCDWSH/SS bears a thiol/disulfide unit at the wide rim of ß-cyclodextrin as a client recognition unit. ßCDWSH/SS shows promiscuous binding to client proteins, mitigates protein aggregation, and accelerates disulfide-bond formation. In contrast, positioning a thiol/disulfide unit at the narrow rim of ß-cyclodextrin promotes folding less effectively through preferential interactions at specific residues, resulting in aggregation. The combination of promiscuous client-binding and redox reactivity is effective for the design of synthetic folding promoters. ßCDWSH/SS accelerates oxidative protein folding at highly condensed sub-millimolar protein concentrations.
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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article
Texto completo
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XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2024 Tipo de documento: Article