Department of Biomedical Sciences University of Padova and CNR Institute of Neuroscience, Padova, Italy.
PLoS One. 2011 Jan 28;6(1):e16280. doi: 10.1371/journal.pone.0016280.
Antamanide is a cyclic decapeptide derived from the fungus Amanita phalloides. Here we show that antamanide inhibits the mitochondrial permeability transition pore, a central effector of cell death induction, by targeting the pore regulator cyclophilin D. Indeed, (i) permeability transition pore inhibition by antamanide is not additive with the cyclophilin D-binding drug cyclosporin A, (ii) the inhibitory action of antamanide on the pore requires phosphate, as previously shown for cyclosporin A; (iii) antamanide is ineffective in mitochondria or cells derived from cyclophilin D null animals, and (iv) abolishes CyP-D peptidyl-prolyl cis-trans isomerase activity. Permeability transition pore inhibition by antamanide needs two critical residues in the peptide ring, Phe6 and Phe9, and is additive with ubiquinone 0, which acts on the pore in a cyclophilin D-independent fashion. Antamanide also abrogates mitochondrial depolarization and the ensuing cell death caused by two well-characterized pore inducers, clotrimazole and a hexokinase II N-terminal peptide. Our findings have implications for the comprehension of cyclophilin D activity on the permeability transition pore and for the development of novel pore-targeting drugs exploitable as cell death inhibitors.
安塔曼肽是一种源自毒蕈鹅膏(Amanita phalloides)的环十肽。在这里,我们发现安塔曼肽通过靶向孔调节蛋白亲环素 D 来抑制线粒体通透性转换孔,这是细胞死亡诱导的中心效应因子。事实上,(i)安塔曼肽对通透性转换孔的抑制作用与亲环素 D 结合药物环孢菌素 A 没有叠加作用,(ii)安塔曼肽对孔的抑制作用需要磷酸盐,如环孢菌素 A 先前所示;(iii)安塔曼肽在亲环素 D 缺失动物的线粒体或细胞中无效,和(iv)抑制 CyP-D 肽基脯氨酰顺反异构酶活性。安塔曼肽对通透性转换孔的抑制作用需要肽环中的两个关键残基,苯丙氨酸 6 和苯丙氨酸 9,并且与泛醌 0 相加,泛醌 0 以亲环素 D 非依赖性方式作用于孔。安塔曼肽还可消除由两种特征明确的孔诱导剂,克霉唑和己糖激酶 II N 端肽引起的线粒体去极化和随后的细胞死亡。我们的研究结果对理解亲环素 D 在通透性转换孔上的活性以及开发可作为细胞死亡抑制剂的新型靶向孔药物具有重要意义。