抑制 Trk 可减少 SK-ES-1 尤文肉瘤细胞中瘤球的形成并改变干性标志物的表达

Rafael Pereira dos Santos, Bruna Almeida dos Santos, L. Gregianin, André Tessainer Brunetto, Algemir Lunardi Brunetto, Rafael Roesler, Caroline Brunetto de Farias
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摘要

简介尤文肉瘤(ES)是一种侵袭性极强的儿童癌症,其特点是染色体易位导致编码EWS RNA结合蛋白1(EWSR1)的基因与ETS家族的一个基因(最常见的是FLI-1)融合,形成EWS-FLI1异常转录因子。ES肿瘤可包含具有癌症干细胞(CSC)特征的亚群细胞,这些细胞表达包括CD133、OCT4(八聚体结合转录因子4)和NANOG在内的干性标志物,并显示出形成可能富含CSC的肿瘤球的能力。肌球蛋白受体激酶(Trk)家族的神经营养素(NT)受体(TrkA、TrkB和TrkC)可能在刺激ES进展中发挥作用,但它们在CSCs中可能发挥的作用仍不清楚。研究目的验证Trks抑制对肿瘤球形成以及干标志物基因表达的影响。方法解离细胞,用补充培养基诱导瘤球形成,并进行K252a处理。提取 RNA 后,通过 qPCR 分析靶基因 Prom1 (CD133)、OCT4 (POU5F1)、SOX2 和 Musashi-1 (MSI1) 的 mRNA 表达水平。结果显示泛Trk抑制剂K252a(100或500 mM)阻碍了人SK-ES-1 ES细胞培养物中瘤球的形成。K252a 还降低了 Prom1(CD133 编码基因)的 mRNA 表达,同时提高了 OCT4 的表达。没有观察到 SOX2 或 Musashi-1 的 mRNA 水平发生变化。结论这些发现提供了首个证据,表明Trk活性可影响ES细胞的干性。
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Trk Inhibition Reduces Tumorsphere Formation and Changes Expression of Stemness Markers in SK-ES-1 Ewing Sarcoma Cells
Introduction: Ewing sarcoma (ES) is a highly aggressive type of childhood cancer characterized by a chromosomal translocation resulting in fusions between the gene encoding EWS RNA Binding Protein 1 (EWSR1) and one gene of the ETS family, most frequently FLI-1, resulting in the EWS-FLI1 aberrant transcription factor. ES tumors can contain a subpopulation of cells showing cancer stem cell (CSC) features, which express stemness markers including CD133, OCT4 (Octamer-binding transcription factor 4), and NANOG, and display capacity to form tumorspheres likely enriched in CSCs. Neurotrophin (NT) receptors of the tropomyosin receptor kinase (Trk) family (TrkA, TrkB, and TrkC) may play a role in stimulating ES progression, but their possible role in CSCs remains unknown. Objective: To verify the effect of Trks inhibition on the formation of tumorspheres as well as the gene expression of stem markers. Method: The cells were dissociated and the formation of spheres was induced with supplemented culture medium and the K252a treatment was performed. After RNA extraction, mRNA expression levels of target genes Prom1 (CD133), OCT4 (POU5F1), SOX2, and Musashi-1 (MSI1) were analyzed by qPCR. Results: The pan-Trk inhibitor K252a (100 or 500 mM) hindered tumorsphere formation in human SK-ES-1 ES cell cultures. K252a also reduced mRNA expression of Prom1 (CD133-coding gene) while enhancing expression of OCT4. No changes in mRNA levels of SOX2 or Musashi-1 were observed. Conclusion: These findings provide the first evidence suggesting that Trk activity can influence stemness in ES cells.
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