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Suppression of human brain tumor with interference RNA specific for tenascin-C.

机译:用针对腱生蛋白-C的干扰RNA抑制人脑肿瘤。

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摘要

Glioblastoma multiforme (GBM) accounts for approximately 12-15% of intracranial neoplasms. The GBM remains refractory to therapy because of tumor heterogeneity, local invasion, and non-uniform vascular permeability to drugs. Patients with GBM have the median survival of approximately 8-10 months, and for those cases where tumor recurs, the average time of tumor progression after therapy is only eight weeks. A combination of different treatment modes as surgery and chemo- or/and radiotherapy extend survival only for a short time, if any. Recently, tenascin-C (TN-C) as a dominant epitope in glioblastoma has been discovered. It is transiently expressed during organogenesis, absent or much reduced in most fully developed organs, but reappears under pathological conditions such as infection, inflammation, or tumorigenesis. It was found that the intensity of TN-C staining correlates with the tumor grade and that the strongest staining indicates poor prognosis.
机译:多形胶质母细胞瘤(GBM)约占颅内肿瘤的12-15%。由于肿瘤异质性,局部浸润和药物的不均匀血管通透性,GBM仍然难以治疗。 GBM患者的中位生存期约为8-10个月,对于那些肿瘤复发的患者,治疗后平均肿瘤进展时间仅为8周。手术,化学疗法和/或放射疗法等不同治疗模式的组合只能延长生存时间(如果有)。最近,已经发现腱生蛋白-C(TN-C)作为胶质母细胞瘤中的优势表位。它在器官发生过程中短暂表达,在最发达的器官中不存在或减少很多,但在诸如感染,炎症或肿瘤发生等病理条件下重新出现。已经发现TN-C染色的强度与肿瘤的等级有关,最强的染色表明预后不良。

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