Fas/CD95 信号传导中 caspase-10 依赖性细胞死亡不会被 caspase 抑制剂 zVAD-fmk 阻断。
Caspase-10-dependent cell death in Fas/CD95 signalling is not abrogated by caspase inhibitor zVAD-fmk.
机构信息
U858 INSERM (Institut National de la Santé et de la Recherche Médicale), Département Cancer, Equipe 14, Toulouse, France.
出版信息
PLoS One. 2010 Oct 26;5(10):e13638. doi: 10.1371/journal.pone.0013638.
BACKGROUND
Upon CD95/Fas ligation, the initiator caspase-8 is known to activate effector caspases leading to apoptosis. In the presence of zVAD-fmk, a broad-spectrum caspase inhibitor, Fas engagement can also trigger an alternative, non-apoptotic caspase-independent form of cell death, which is initiated by RIP1. Controversy exists as to the ability of caspase-10 to mediate cell death in response to FasL (CD95L or CD178). Herein, the role of caspase-10 in FasL-induced cell death has been re-evaluated.
METHODOLOGY AND PRINCIPAL FINDINGS
The present study shows that FasL-induced cell death was completely impaired in caspase-8- and caspase-10-doubly deficient (I9-2e) Jurkat leukaemia T-cell lines. Over-expressing of either caspase-8 or caspase-10 in I9-2e cells triggered cell death and restored sensitivity to FasL, further arguing for a role of both initiator caspases in Fas apoptotic signalling. In the presence of zVAD-fmk, FasL triggered an alternative form of cell death similarly in wild-type (A3) and in caspase-8-deficient Jurkat cells expressing endogenous caspase-10 (clone I9-2d). Cell death initiated by Fas stimulation in the presence of zVAD-fmk was abrogated in I9-2e cells as well as in HeLa cells, which did not express endogenous caspase-10, indicating that caspase-10 somewhat participates in this alternative form of cell death. Noteworthy, ectopic expression of caspase-10 in I9-2e and HeLa cells restored the ability of FasL to trigger cell death in the presence of zVAD-fmk. As a matter of fact, FasL-triggered caspase-10 processing still occurred in the presence of zVAD-fmk.
CONCLUSIONS AND SIGNIFICANCE
Altogether, these data provide genetic evidence for the involvement of initiator caspase-10 in FasL-induced cell death and indicate that zVAD-fmk does not abrogate caspase-10 processing and cytotoxicity in Fas signalling. Our study also questions the existence of an alternative caspase-independent cell death pathway in Fas signalling.
背景
CD95/Fas 配体结合后,起始半胱天冬酶-8 被认为能激活效应半胱天冬酶,导致细胞凋亡。在广谱半胱天冬酶抑制剂 zVAD-fmk 的存在下,Fas 结合也能触发一种替代的、无细胞凋亡的半胱天冬酶非依赖性的细胞死亡形式,这种形式由 RIP1 引发。关于半胱天冬酶-10 在 FasL(CD95L 或 CD178)反应中介导细胞死亡的能力存在争议。本文重新评估了半胱天冬酶-10 在 FasL 诱导的细胞死亡中的作用。
方法和主要发现
本研究表明,半胱天冬酶-8 和半胱天冬酶-10 双重缺陷(I9-2e)Jurkat 白血病 T 细胞系中 FasL 诱导的细胞死亡完全受损。在 I9-2e 细胞中过表达半胱天冬酶-8 或半胱天冬酶-10 会触发细胞死亡,并恢复对 FasL 的敏感性,进一步证明这两种起始半胱天冬酶在 Fas 凋亡信号转导中发挥作用。在 zVAD-fmk 的存在下,FasL 以类似的方式在野生型(A3)和表达内源性半胱天冬酶-10 的 caspase-8 缺陷型 Jurkat 细胞(克隆 I9-2d)中触发另一种形式的细胞死亡。在 I9-2e 细胞和不表达内源性半胱天冬酶-10 的 HeLa 细胞中,zVAD-fmk 存在时 Fas 刺激引发的细胞死亡被阻断,表明半胱天冬酶-10 参与了这种替代形式的细胞死亡。值得注意的是,I9-2e 和 HeLa 细胞中外源表达半胱天冬酶-10 恢复了 FasL 在 zVAD-fmk 存在下触发细胞死亡的能力。事实上,在 zVAD-fmk 的存在下,FasL 触发的半胱天冬酶-10 加工仍然发生。
结论和意义
总之,这些数据为起始半胱天冬酶-10 参与 FasL 诱导的细胞死亡提供了遗传证据,并表明 zVAD-fmk 并不能阻断 Fas 信号转导中半胱天冬酶-10 的加工和细胞毒性。我们的研究还质疑 Fas 信号转导中是否存在替代的无半胱天冬酶依赖性细胞死亡途径。
Zotero 插件