INSERM U916 VINCO, Institut Bergonié, Bordeaux 33076 France.
Oncogene. 2010 Mar 25;29(12):1717-9. doi: 10.1038/onc.2009.519. Epub 2010 Jan 25.
Beclin 1 has a key role in the initiation of autophagy, a process of self-cannibalism in which cytoplasmic constituents are sequestered and targeted for lysosomal degradation. In a recent issue of Cell Death & Disease, Wirawan et al. report the significant finding that caspases can cleave Beclin 1, thereby destroying its pro-autophagic activity. Moreover, the C-terminal fragment of Beclin 1 that results from this cleavage acquires a new function and can amplify mitochondrion-mediated apoptosis. Of note, the BH3 domain of Beclin 1 remains within the N-terminal fragment, which has no detectable pro-apoptotic activity. These findings provide important insights into the molecular cross talk between autophagy and apoptosis.
Beclin 1 在自噬的起始过程中起着关键作用,自噬是一种自我吞噬的过程,其中细胞质成分被隔离并靶向溶酶体降解。在最近一期的《细胞死亡与疾病》杂志上,Wirawan 等人报告了一个重要发现,即半胱天冬酶可以切割 Beclin 1,从而破坏其促进自噬的活性。此外,这种切割产生的 Beclin 1 的 C 末端片段获得了新的功能,可以放大线粒体介导的细胞凋亡。值得注意的是,Beclin 1 的 BH3 结构域保留在无明显促凋亡活性的 N 末端片段中。这些发现为自噬和细胞凋亡之间的分子串扰提供了重要的见解。
