Gajate Consuelo, Gonzalez-Camacho Fernando, Mollinedo Faustino
Instituto de Biología Molecular y Celular del Cáncer, Centro de Investigación del Cáncer, Consejo Superior de Investigaciones Científicas, Universidad de Salamanca, Salamanca, Spain.
PLoS One. 2009;4(4):e5044. doi: 10.1371/journal.pone.0005044. Epub 2009 Apr 7.
Recent evidence suggests that co-clustering of Fas/CD95 death receptor and lipid rafts plays a major role in death receptor-mediated apoptosis.
METHODOLOGY/PRINCIPAL FINDINGS: By a combination of genetic, biochemical, and ultrastructural approaches, we provide here compelling evidence for the involvement of lipid raft aggregates containing recruited Fas/CD95 death receptor, Fas-associated death domain-containing protein (FADD), and procaspase-8 in the induction of apoptosis in human T-cell leukemia Jurkat cells by the antitumor drug edelfosine, the prototype compound of a promising family of synthetic antitumor lipids named as synthetic alkyl-lysophospholipid analogues. Co-immunoprecipitation assays revealed that edelfosine induced the generation of the so-called death-inducing signaling complex (DISC), made up of Fas/CD95, FADD, and procaspase-8, in lipid rafts. Electron microscopy analyses allowed to visualize the formation of raft clusters and their co-localization with DISC components Fas/CD95, FADD, and procaspase-8 following edelfosine treatment of Jurkat cells. Silencing of Fas/CD95 by RNA interference, transfection with a FADD dominant-negative mutant that blocks Fas/CD95 signaling, and specific inhibition of caspase-8 prevented the apoptotic response triggered by edelfosine, hence demonstrating the functional role of DISC in drug-induced apoptosis. By using radioactive labeled edelfosine and a fluorescent analogue, we found that edelfosine accumulated in lipid rafts, forming edelfosine-rich membrane raft clusters in Jurkat leukemic T-cells. Disruption of these membrane raft domains abrogated drug uptake and drug-induced DISC assembly and apoptosis. Thus, edelfosine uptake into lipid rafts was critical for the onset of both co-aggregation of DISC in membrane rafts and subsequent apoptotic cell death.
CONCLUSIONS/SIGNIFICANCE: This work shows the involvement of DISC clusters in lipid raft aggregates as a supramolecular and physical entity responsible for the induction of apoptosis in leukemic cells by the antitumor drug edelfosine. Our data set a novel framework and paradigm in leukemia therapy, as well as in death receptor-mediated apoptosis.
最近的证据表明,Fas/CD95死亡受体与脂筏的共聚集在死亡受体介导的细胞凋亡中起主要作用。
方法/主要发现:通过基因、生化和超微结构方法的结合,我们在此提供了令人信服的证据,证明含有募集的Fas/CD95死亡受体、含Fas相关死亡结构域蛋白(FADD)和procaspase-8的脂筏聚集体参与了抗肿瘤药物依地福新(一种名为合成烷基溶血磷脂类似物的有前景的合成抗肿瘤脂质家族的原型化合物)诱导人T细胞白血病Jurkat细胞凋亡的过程。免疫共沉淀分析表明,依地福新诱导了脂筏中由Fas/CD95、FADD和procaspase-8组成的所谓死亡诱导信号复合物(DISC)的生成。电子显微镜分析能够观察到依地福新处理Jurkat细胞后脂筏簇的形成及其与DISC组分Fas/CD95、FADD和procaspase-8的共定位。通过RNA干扰使Fas/CD95沉默、用阻断Fas/CD95信号的FADD显性负性突变体转染以及对caspase-8的特异性抑制,均能阻止依地福新触发的凋亡反应,从而证明了DISC在药物诱导凋亡中的功能作用。通过使用放射性标记的依地福新和一种荧光类似物,我们发现依地福新在脂筏中积累,在Jurkat白血病T细胞中形成富含依地福新的膜脂筏簇。破坏这些膜脂筏结构域可消除药物摄取以及药物诱导的DISC组装和凋亡。因此,依地福新摄取到脂筏中对于膜脂筏中DISC的共聚集以及随后的凋亡细胞死亡的起始至关重要。
结论/意义:这项工作表明DISC簇参与脂筏聚集体,作为一种超分子和物理实体,负责抗肿瘤药物依地福新诱导白血病细胞凋亡。我们的数据为白血病治疗以及死亡受体介导的细胞凋亡建立了一个新的框架和范例。
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