Golks Alexander, Brenner Dirk, Fritsch Cornelius, Krammer Peter H, Lavrik Inna N
Division of Immunogenetics, Tumorimmunology Program, German Cancer Research Center, Im Neuenheimer Feld 280, D-69120 Heidelberg, Germany.
J Biol Chem. 2005 Apr 15;280(15):14507-13. doi: 10.1074/jbc.M414425200. Epub 2005 Feb 8.
c-FLIPs (c-FLICE inhibitory proteins) play an essential role in regulation of death receptor-induced apoptosis. Multiple splice variants of c-FLIP have been described on the mRNA level; so far only two of them, c-FLIP(L) and c-FLIP(S,) had been found to be expressed at the protein level. In this report, we reveal the endogenous expression of a third isoform of c-FLIP. We demonstrate its presence in a number of T and B cell lines as well as in primary human T cells. We identified this isoform as c-FLIP(R), a death effector domain-only splice variant previously identified on the mRNA level. Impor-/tantly, c-FLIP(R) is recruited to the CD95 (Fas/APO-1) death-inducing signaling complex upon CD95 stimulation. Several properties of c-FLIP(R) are similar to c-FLIP(S): both isoforms have a short half-life, a similar pattern of expression during activation of primary human T cells, and are strongly induced in T cells upon CD3/CD28 costimulation. Taken together, our data demonstrate endogenous expression of c-FLIP(R) and similar roles of c-FLIP(R) and c-FLIP(S) isoforms in death receptor-mediated apoptosis.
c-FLIPs(c-FLICE抑制蛋白)在死亡受体诱导的细胞凋亡调控中发挥着重要作用。在mRNA水平上已描述了c-FLIP的多种剪接变体;到目前为止,仅发现其中两种,即c-FLIP(L)和c-FLIP(S)在蛋白质水平上表达。在本报告中,我们揭示了c-FLIP的第三种异构体的内源性表达。我们证明了它在许多T和B细胞系以及原代人T细胞中的存在。我们将这种异构体鉴定为c-FLIP(R),一种先前在mRNA水平上鉴定出的仅含死亡效应结构域的剪接变体。重要的是,在CD95刺激后,c-FLIP(R)被招募到CD95(Fas/APO-1)死亡诱导信号复合物中。c-FLIP(R)的几个特性与c-FLIP(S)相似:这两种异构体都具有较短的半衰期,在原代人T细胞激活过程中的表达模式相似,并且在T细胞经CD3/CD28共刺激后被强烈诱导。综上所述,我们的数据证明了c-FLIP(R)的内源性表达以及c-FLIP(R)和c-FLIP(S)异构体在死亡受体介导的细胞凋亡中发挥的相似作用。
