From the German Cancer Research Center, BioQuant, ImNeuenheimer Feld 267, 69120 Heidelberg, Germany.
J Biol Chem. 2013 Nov 15;288(46):33241-52. doi: 10.1074/jbc.M113.512087. Epub 2013 Oct 7.
The Bcl-2 proapoptotic proteins Bax and Bak mediate the permeabilization of the mitochondrial outer membrane during apoptosis. Current models consider that Bax and Bak form pores at the mitochondrial outer membrane that are responsible for the release of cytochrome c and other larger mitochondrial apoptotic factors (i.e. Smac/DIABLO, AIF, and endoglycosidase G). However, the properties and nature of Bax/Bak apoptotic pores remain enigmatic. Here, we performed a detailed analysis of the membrane permeabilizing activity of Bax and Bak at the single vesicle level. We directly visualized that cBid-activated Bax and BakΔC21 can form membrane pores large enough to release not only cytochrome c, but also allophycocyanine, a protein of 104 kDa. Interestingly, the size of Bax and BakΔC21 pores is not constant, as typically observed in purely proteinaceous channels, but evolves with time and depends on protein concentration. We found that Bax and BakΔC21 formed long-lived pores, whose areas changed with the amount of Bax/BakΔC21 but not with cardiolipin concentration. Altogether, our results demonstrate that Bax and BakΔC21 follow similar mechanisms of membrane permeabilization characterized by the formation of protein-permeable pores of dynamic size, in agreement with the proteolipidic nature of these apoptotic pores.
Bcl-2 促凋亡蛋白 Bax 和 Bak 在细胞凋亡过程中介导线粒体外膜的通透化。目前的模型认为,Bax 和 Bak 在线粒体膜上形成孔道,负责细胞色素 c 和其他较大的线粒体凋亡因子(即 Smac/DIABLO、AIF 和内糖苷酶 G)的释放。然而,Bax/Bak 凋亡孔的特性和性质仍然是个谜。在这里,我们在单个囊泡水平上对 Bax 和 Bak 的膜通透活性进行了详细分析。我们直接观察到,cBid 激活的 Bax 和 BakΔC21 可以形成足够大的膜孔,不仅可以释放细胞色素 c,还可以释放别藻蓝蛋白,一种分子量为 104 kDa 的蛋白。有趣的是,Bax 和 BakΔC21 孔的大小不是恒定的,如在纯蛋白通道中通常观察到的那样,而是随时间演变,并取决于蛋白质浓度。我们发现,Bax 和 BakΔC21 形成了长寿命的孔,其面积随 Bax/BakΔC21 的量而变化,但不受心磷脂浓度的影响。总之,我们的结果表明,Bax 和 BakΔC21 遵循类似的膜通透化机制,其特征是形成动态大小的蛋白渗透性孔,这与这些凋亡孔的蛋白脂性质一致。
