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DNM3, p65 and p53 from exosomes represent potential clinical diagnosis markers for glioblastoma multiforme

机译:Exosomes的DNM3,P65和P53代表了胶质母细胞瘤多形态临床诊断标志物

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Glioblastoma multiforme (GBM) is the most aggressive and deadly primary brain cancer that arises from astrocytes and classified as grade IV. Recently, exosomes have been reported as an essential mediator in diverse cancer carcinogenesis and metastasis. However, their role in GBM is still unclear. In this study, we aimed to investigate whether blood exosomes can be potential clinical diagnostic markers for GBM. We used a xenograft orthotopic mouse model to detect the differentially expressed genes in the brain and blood exosomes of original/recurrent GBM. We found that recurrent GBM had stronger growth capacity and lethality than original GBM in the mouse model. A gene microarray of original tumors and blood exosomes from GBM orthotopic xenografts results showed that DNM3, p65 and CD117 expressions increased, whereas PTEN and p53 expressions decreased in both original tumors and blood exosomes. In the recurrent GBM tumor model, DNM3 and p65 showed increased expressions, whereas ST14 and p53 showed decreased expressions in tumor and blood exosomes of the recurrent GBM mouse model. In summary, we found that DNM3, p65 and p53 had a similar trend in brain and blood exosomes both for original and recurrent GBM, and could serve as potential clinical diagnostic markers for GBM.
机译:胶质母细胞瘤多形形(GBM)是从星形胶质细胞产生的最具侵略性和致命的主要脑癌,并被归类为IV级。最近,据报道,外泌体作为各种癌症致癌和转移的必需调解员。然而,他们在GBM中的作用尚不清楚。在这项研究中,我们旨在调查血液外泌体是否可以是GBM的潜在临床诊断标志物。我们使用了异种移植物原位小鼠模型来检测原始/复发性GBM的脑和血外肌肉中的差异表达基因。我们发现经常性GBM在小鼠模型中具有比原始GBM更强的增长能力和致命性。来自GBM原位卵黄移植物的原始肿瘤的基因微阵列和来自GBM的血管瘤结果结果表明,DNM3,P65和CD117表达增加,而PTEN和P53表达在原始肿瘤和血液外瘤中减少。在复发性GBM肿瘤模型中,DNM3和P65显示出较高的表达,而ST14和P53表现出肿瘤和复发性GBM小鼠模型的肿瘤和血液外瘤的表达减少。总之,我们发现DNM3,P65和P53在脑和血液外部患有类似的脑外的GBM,并且可以作为GBM的潜在临床诊断标志物。

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