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Loperamide pimozide and STF-62247 trigger autophagy-dependent cell death in glioblastoma cells

机译:洛哌丁胺匹莫唑和STF-62247触发胶质母细胞瘤细胞中自噬依赖性细胞死亡

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Autophagy is a well-described degradation mechanism that promotes cell survival upon nutrient starvation and other forms of cellular stresses. In addition, there is growing evidence showing that autophagy can exert a lethal function via autophagic cell death (ACD). As ACD has been implicated in apoptosis-resistant glioblastoma (GBM), there is a high medical need for identifying novel ACD-inducing drugs. Therefore, we screened a library containing 70 autophagy-inducing compounds to induce ATG5-dependent cell death in human MZ-54 GBM cells. Here, we identified three compounds, i.e. loperamide, pimozide, and STF-62247 that significantly induce cell death in several GBM cell lines compared to CRISPR/Cas9-generated ATG5- or ATG7-deficient cells, pointing to a death-promoting role of autophagy. Further cell death analyses conducted using pharmacological inhibitors revealed that apoptosis, ferroptosis, and necroptosis only play minor roles in loperamide-, pimozide- or STF-62247-induced cell death. Intriguingly, these three compounds induce massive lipidation of the autophagy marker protein LC3B as well as the formation of LC3B puncta, which are characteristic of autophagy. Furthermore, loperamide, pimozide, and STF-62247 enhance the autophagic flux in parental MZ-54 cells, but not in ATG5 or ATG7 knockout (KO) MZ-54 cells. In addition, loperamide- and pimozide-treated cells display a massive formation of autophagosomes and autolysosomes at the ultrastructural level. Finally, stimulation of autophagy by all three compounds is accompanied by dephosphorylation of mammalian target of rapamycin complex 1 (mTORC1), a well-known negative regulator of autophagy. In summary, our results indicate that loperamide, pimozide, and STF-62247 induce ATG5- and ATG7-dependent cell death in GBM cells, which is preceded by a massive induction of autophagy. These findings emphasize the lethal function and potential clinical relevance of hyperactivated autophagy in GBM.
机译:自噬是众所周知的降解机制,可在营养不足和其他形式的细胞应激时促进细胞存活。另外,越来越多的证据表明自噬可以通过自噬细胞死亡(ACD)发挥致命作用。由于ACD与抗凋亡胶质母细胞瘤(GBM)有关,因此对鉴定新型ACD诱导药物的医疗需求很高。因此,我们筛选了包含70种自噬诱导化合物的文库,以诱导人MZ-54 GBM细胞中ATG5依赖性细胞死亡。在这里,我们确定了三种化合物,即洛哌丁胺,匹莫齐和STF-62247,与CRISPR / Cas9产生的ATG5或ATG7缺陷型细胞相比,它们可以在几种GBM细胞系中显着诱导细胞死亡,这表明自噬具有促进死亡的作用。使用药理学抑制剂进行的进一步细胞死亡分析表明,凋亡,肥大症和坏死病仅在洛哌丁胺,匹莫齐德或STF-62247诱导的细胞死亡中起较小作用。有趣的是,这三种化合物诱导自噬标记蛋白LC3B大量脂质化以及LC3B点状的形成,这是自噬的特征。此外,洛哌丁胺,匹莫齐和STF-62247可增强亲本MZ-54细胞的自噬通量,但不会增强ATG5或ATG7敲除(KO)MZ-54细胞的自噬通量。此外,洛哌丁胺和匹莫唑治疗的细胞在超微结构水平上显示出大量自噬体和溶酶体的形成。最后,所有三种化合物对自噬的刺激都伴随着雷帕霉素复合物1(mTORC1)的哺乳动物靶点的去磷酸化,雷帕霉素复合物1(mTORC1)是众所周知的自噬负调节剂。总之,我们的结果表明,洛哌丁胺,匹莫齐和STF-62247诱导GBM细胞中ATG5-和ATG7依赖性细胞死亡,然后大量诱导自噬。这些发现强调了GBM中超活化自噬的致死功能和潜在的临床意义。

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