Torriglia Alicia, Lepretre Chloe
Universite Pierre et Marie Curie-Paris 6, Paris, F-75006 France.
Front Biosci (Landmark Ed). 2009 Jun 1;14(13):4836-47. doi: 10.2741/3572.
Caspase activation has been seen, for several years, as the biochemical marker of apoptosis. However, in 2005 the Nomenclature Committee on Cell Death (NCCD) established that the 'official' classification of cell death had to rely on morphological criteria owing to the absence of a clear-cut equivalence between structural alterations and biochemical pathways. Actually, the controlled destruction of the cell is coordinated by a proteolytic system involving caspases but also other proteases like cathepsins, calpains and serine proteases. These enzymes participate in an activation cascade that culminates in cleavage of a set of proteins resulting in disassembly of the cell. This disassembling also includes the activation of endonucleases that will destroy a potentially harmful DNA. A caspase-activated DNase performs DNA degradation in caspase-dependent apoptosis, but other endonucleases like L-DNase II or GAAD are activated in caspase-independent apoptosis, allowing the complete dismantling of the cell.
多年来,半胱天冬酶激活一直被视为细胞凋亡的生化标志物。然而,2005年细胞死亡命名委员会(NCCD)确定,由于结构改变与生化途径之间缺乏明确的对应关系,细胞死亡的“官方”分类必须依赖形态学标准。实际上,细胞的可控性破坏是由一个蛋白水解系统协调的,该系统不仅涉及半胱天冬酶,还包括其他蛋白酶,如组织蛋白酶、钙蛋白酶和丝氨酸蛋白酶。这些酶参与一个激活级联反应,最终导致一组蛋白质的切割,从而导致细胞解体。这种解体还包括核酸内切酶的激活,这些核酸内切酶将破坏潜在有害的DNA。一种半胱天冬酶激活的脱氧核糖核酸酶在依赖半胱天冬酶的细胞凋亡中执行DNA降解,但其他核酸内切酶,如L-DNase II或GAAD,在不依赖半胱天冬酶的细胞凋亡中被激活,从而使细胞完全解体。