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  Determinants of BH3 Sequence Specificity for the Disruption of Bcl-xL/cBid Complexes in Membranes

Das, K. K., Shalaby, R., & García-Sáez, A. J. (2017). Determinants of BH3 Sequence Specificity for the Disruption of Bcl-xL/cBid Complexes in Membranes. ACS Chemical Biology, 12(4), 989-1000. doi:10.1021/acschembio.6b01084.

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アイテムのパーマリンク: https://hdl.handle.net/21.11116/0000-000F-3982-E 版のパーマリンク: https://hdl.handle.net/21.11116/0000-000F-3983-D
資料種別: 学術論文

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 作成者:
Das, Kushal Kumar1, 著者
Shalaby, Raed1, 著者
García-Sáez, Ana J.2, 3, 著者                 
所属:
1External Organizations, ou_persistent22              
2Interfaculty Institute of Biochemistry, Eberhard-Karls-Universität Tübingen, Tübingen, Germany, ou_persistent22              
3Max Planck Institute for Intelligent Systems, Stuttgart, Germany, ou_persistent22              

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キーワード: bcl-X Protein, BH3 Interacting Domain Death Agonist Protein, Binding Sites, Cell Membrane, Humans, Molecular Docking Simulation, Molecular Mimicry, Peptides, Protein Binding
 要旨: The prosurvival Bcl-2 proteins exhibit a specific pattern of interactions with BH3-only proteins that determines the cellular dependence on apoptotic stress. This specificity is crucial for the development of BH3 mimetics, a class of anticancer molecules based on the BH3 domain with promising activity in clinical trials. Although complex formation mainly takes place in the mitochondrial outer membrane, most studies so far addressed the interaction between BH3 peptides and truncated Bcl-2 proteins in solution. As a consequence, quantitative understanding of the sequence specificity determinants of BH3 peptides in the membrane environment is missing. Here, we tackle this issue by systematically quantifying the ability of BH3 peptides to compete for the complexes between cBid and Bcl-xL in giant unilamellar vesicles and compare it with solution and mitochondria. We show that the BH3 peptides derived from Hrk, Bim, Bid, and Bad are the most efficient in disrupting cBid/Bcl-xL complexes in the membrane, which correlates with their activity in mitochondria. Our findings support the targeting to the membrane of small molecules that bind Bcl-2 proteins as a strategy to improve their efficiency.

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言語: eng - English
 日付: 2016-12-072017-02-072017-04-07
 出版の状態: 出版
 ページ: 12
 出版情報: -
 目次: -
 査読: 査読あり
 識別子(DOI, ISBNなど): DOI: 10.1021/acschembio.6b01084
BibTex参照ID: das_determinants_2017
 学位: -

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出版物 1

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出版物名: ACS Chemical Biology
  省略形 : ACS Chem. Biol.
種別: 学術雑誌
 著者・編者:
所属:
出版社, 出版地: Washington, D.C. : American Chemical Society
ページ: - 巻号: 12 (4) 通巻号: - 開始・終了ページ: 989 - 1000 識別子(ISBN, ISSN, DOIなど): ISSN: 1554-8929
CoNE: https://pure.mpg.de/cone/journals/resource/1000000000035040