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首页> 外文期刊>Critical reviews in oncology/hematology >Treatment options for malignant gliomas, emphasizing towards new molecularly targeted therapies.
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Treatment options for malignant gliomas, emphasizing towards new molecularly targeted therapies.

机译:恶性神经胶质瘤的治疗选择,重点是新的分子靶向疗法。

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Malignant gliomas (MGs), including glioblastomas and anaplastic astrocytomas are the most common primary brain tumors. Despite treatment advances, the outcome of patients diagnosed with MGs is poor. The current standard treatment protocols for managing these tumors include maximally safe surgical resection, followed by fractioned radiation therapy of the tumor and surrounding brain parenchyma. Until recently, the use of systemic chemotherapy was restricted and ineffective, due to the fact that the blood brain barrier inhibits the adequate therapeutic concentrations of most chemotherapeutic agents into the tumor and peritumoral area. Genetic transformation, like the expression of the DNA repair enzyme methylguanine methyltransferase (MGMT) and specific characteristics of these neoplasms are also causal factors, accounting for the development of treatment resistance to standard chemotherapy options with alkylating compounds. Recent advances, mostly, in thorough understanding of the complex molecular pathogenesis of MGs have led to arousal of rational development of new molecularly targeted treatment options that simultaneously affect multiple signalling pathways. Currently, several molecularly targeted agents, like tyrosine kinase and growth factor inhibitors have been tested in clinical trials to establish future directions in the therapy of MGs. A number of novel targeted strategies, including among others radio-immuno and ligand-toxin conjugates and RNA-based therapies, are also under investigation. We herein review and discuss the standard treatment options and recent advances in the therapy of MGs, with emphasis on the current knowledge towards the molecular pathogenesis of MGs as well as molecularly targeted therapies. We also highlight areas of future research.
机译:恶性神经胶质瘤(MG),包括成胶质细胞瘤和间变性星形细胞瘤是最常见的原发性脑肿瘤。尽管治疗有所进步,但被诊断患有重症肌无力的患者的预后仍然很差。当前处理这些肿瘤的标准治疗方案包括最大程度的安全手术切除,然后进行肿瘤和周围脑实质的分级放射治疗。直到最近,由于血脑屏障抑制了大多数化学治疗剂进入肿瘤和肿瘤周围区域的适当治疗浓度,因此全身化学疗法的使用受到限制和无效。遗传转化,例如DNA修复酶甲基鸟嘌呤甲基转移酶(MGMT)的表达和这些肿瘤的特定特征,也都是因果关系,说明了对烷基化化合物对标准化学疗法的耐受性。最近的进展,主要是在透彻了解MGs的复杂分子发病机理方面,已引起对同时影响多种信号通路的新型分子靶向治疗选择的合理开发。当前,已经在临床试验中测试了几种分子靶向药物,例如酪氨酸激酶和生长因子抑制剂,以确立MG治疗的未来方向。许多新颖的靶向策略,包括放射免疫和配体毒素偶联物以及基于RNA的疗法,也在研究之中。我们在这里回顾和讨论MGs治疗的标准治疗选择和最新进展,重点是针对MGs分子发病机理以及分子靶向疗法的当前知识。我们还将重点介绍未来的研究领域。

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