ID | 109894 |
タイトルヨミ | UCP3 ト Hax-1 ノ ソウゴ サヨウ ニヨル ミトコンドリア ノ カルシウム ノ ウド ノ チョウセツ
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タイトル別表記 | The interaction between uncoupling protein3 and Hax-1 is regulated by calcium ion in mitochondria
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著者 |
春名, 真里江
徳島大学大学院ヘルスバイオサイエンス研究部生体栄養学
平坂, 勝也
長崎大学水産学部食品栄養学
冨田, 知里
徳島大学大学院ヘルスバイオサイエンス研究部生体栄養学
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キーワード | mitochondria
calcium ion
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資料タイプ |
学術雑誌論文
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抄録 | Mitochondrial Ca2+ plays an important role in the regulations of various cellular functions. Uncoupling protein 3 (UCP3) is primarily expressed in the inner membrane of skeletal muscle mitochondria. Recently, it has been reported that UCP3 is associated with Ca2+ uptake into mitochondria. However, the mechanisms by which UCP3 regulates mitochondrial Ca2+ uptake are not well understood. Here we report that UCP3interacts with HS‐1associated protein X‐1 (Hax‐1), an anti-apoptotic protein that is localized in mitochondria, which is involved in cellular responses to Ca2+. The hydrophilic sequences within the loop2, matrix-localized hydrophilic domain of mouse UCP3are necessary for binding to Hax‐1of the C-terminal domain in adjacent to mitochondrial innermembrane. Interestingly, interaction of these proteins occurs the calciumdependent manner. Moreover, NMR spectrum of the C-terminal domain of Hax‐1was dramatically changed by removal of Ca2+, suggesting that the C-terminal domain of Hax‐1 underwent a Ca2+-induced conformation change. In the Ca2+-free states, C-terminal Hax‐1 didn’t change the structure, suggesting that Ca2+ binding may induce the change of protein structure of Hax‐1 C-terminus. These studies identify a novel UCP3‐Hax‐1complex regulates the influx of Ca2+ into mitochondria. Thus, the efficacy of UCP3‐Hax‐1in mitochondrial calcium regulation may provide a novel therapeutic approach against mitochondrial dysfunction-related disease.
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掲載誌名 |
四国医学雑誌
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ISSN | 00373699
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cat書誌ID | AN00102041
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出版者 | 徳島医学会
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巻 | 70
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号 | 5-6
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開始ページ | 149
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終了ページ | 154
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並び順 | 149
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発行日 | 2014-12-25
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備考 | P.149著者名日本語表記では「真板 綾子」となっているが、P.154英語表記では「Ayako Ohno」となっている。
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フルテキストファイル | |
言語 |
jpn
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著者版フラグ |
出版社版
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部局 |
医学系
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