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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Interaction of the C-terminal domain of Bcl-2 family proteins with model membranes
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Interaction of the C-terminal domain of Bcl-2 family proteins with model membranes

机译:Bcl-2家族蛋白的C末端域与模型膜的相互作用

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Bcl-2 family proteins are involved in the cell homeostasis by regulating programmed cell death. Some of these proteins promote apoptosis, while others inhibit the same process. The C-terminal hydrophobic domain of some of these proteins is predicted to be involved in anchoring them to a variety of cell membranes, such as mitochondrial, endoplasmic reticulum and nuclear membranes. We have used five synthetic peptides imitating the C-terminal domain from both anti-apoptotic (Bcl-2) and pro-apoptotic members (Bak, Bax, and two mutants of this last protein) of this family to study their interaction with model membranes. Some differences were detected in the interaction with these peptides. The addition of all the peptides to large unilamellar vesicles destabilized them and released encapsulated carboxyfluorescein to different degrees, so that fluidity and the increase in negative curvature favoured the extent in the release of carboxyfluorescein. Bcl-2-C and Bax-C peptides produced the highest release levels in most cases, while BaxS184K-C was the least efficient in this respect. These results indicate that these C-terminal domains are able to insert themselves in the membranes, each in a different way that is probably related with their different way which can be related to their differing locations within the cell and their different roles in regulating apoptosis. (c) 2007 Elsevier B.V. All rights reserved.
机译:Bcl-2家族蛋白通过调节程序性细胞死亡而参与细胞稳态。这些蛋白质中的一些促进细胞凋亡,而其他一些则抑制相同的过程。据预测,其中一些蛋白质的C端疏水结构域将其锚定在各种细胞膜上,例如线粒体,内质网和核膜。我们已经使用了五个合成的肽来模拟该家族的抗凋亡成员(Bcl-2)和促凋亡成员(Bak,Bax和最后一个蛋白质的两个突变体)的C末端结构域,以研究它们与模型膜的相互作用。在与这些肽的相互作用中检测到一些差异。将所有肽添加到大的单层囊泡中会使它们不稳定,并以不同程度释放胶囊化的羧基荧光素,因此流动性和负曲率的增加有利于羧基荧光素的释放程度。在大多数情况下,Bcl-2-C和Bax-C肽的释放水平最高,而BaxS184K-C在这方面的效率最低。这些结果表明,这些C端结构域能够以不同的方式将其自身插入膜中,这可能与它们的不同方式有关,这可能与它们在细胞中的不同位置以及它们在调节细胞凋亡中的不同作用有关。 (c)2007 Elsevier B.V.保留所有权利。

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