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PDTM-02. STRESS GRANULES ARE INDUCED BY OXIDATIVE STRESS IN PEDIATRIC BRAIN TUMORS AND PREDICT POOR OUTCOME

机译:PDTM-02。小儿脑肿瘤的氧化性应激和预后不良预示着应激

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摘要

BACKGROUND/OBJECTIVES: Brain tumors represent the most common and aggressive pediatric cancer type, underscoring a dire need for novel therapeutic approaches. Tumors are continually exposed to acute changes in their microenvironment, including oxidative stress. To overcome acute stress, cells form stress granules (SGs), clusters of RNA and RNA-binding proteins (RBPs) that rapidly alter the cellular mRNA translation landscape. Preliminary data indicate that pharmacological inhibition of SG formation blocks the antioxidant response of the transcription factor NRF2 (NFE2L2), impairing pediatric sarcoma invasive and metastatic capacity. We therefore set out to determine if pediatric brain tumors rely on SGs to overcome oxidative stress, and if targeting SGs could represent a therapeutic approach for these tumors.METHODSWe analyzed public databases for links between mRNA expression of the RBP G3BP1 and NFE2L2. Immunohistochemistry (IHC) for G3BP1, NRF2 and oxidative stress markers (4HNE) was performed on atypical theratoid rabdoid tumor (AT/RT), pediatric glioblastoma (pGBM) and ependymoma (EPN) tissue microarrays. AT/RT, pGBM and EPN cell lines were treated with NaAsO2 and H2O2 to induce oxidative stress and SG presence was determined by ImmunoFluorescence for the RBPs G3BP1 and TIA-1.
机译:背景/目的:脑肿瘤代表最常见和侵略性的小儿癌症类型,强调了对新型治疗方法的迫切需求。肿瘤不断暴露于其微环境的急性变化中,包括氧化应激。为了克服急性应激,细胞形成了应激颗粒(SGs​​),RNA和RNA结合蛋白(RBP)簇,它们迅速改变了细胞mRNA的翻译格局。初步数据表明,SG形成的药理抑制作用可阻止转录因子NRF2(NFE2L2)的抗氧化反应,从而损害小儿肉瘤的侵袭和转移能力。因此,我们着手确定小儿脑肿瘤是否依靠SG克服氧化应激,以及靶向SG能否代表这些肿瘤的治疗方法。方法我们分析了公共数据库中RBP G3BP1和NFE2L2 mRNA表达之间的联系。对非典型的类鼻窦类腺瘤(AT / RT),小儿胶质母细胞瘤(pGBM)和室管膜瘤(EPN)组织微阵列进行了G3BP1,NRF2和氧化应激标记物(4HNE)的免疫组织化学(IHC)。用NaAsO2和H2O2处理AT / RT,pGBM和EPN细胞系以诱导氧化应激,并通过免疫荧光法测定RBP G3BP1和TIA-1的SG存在。

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