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Targeted Brain Tumor Treatment: Current Perspectives

机译:靶向脑肿瘤治疗:当前观点

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Brain tumor is associated with poor prognosis. The treatment option is severely limited for a patient with brain tumor, despite great advances in understanding the etiology and molecular biology of brain tumors that have lead to breakthroughs in developing pharmaceutical strategies, and ongoing NCI/Pharma-sponsored clinical trials. We reviewed the literature on molecular targeted agents in preclinical and clinical studies in brain tumor for the past decade, and observed that the molecular targeting in brain tumors is complex. This is because no single gene or protein can be affected by single molecular agent, requiring the use of combination molecular therapy with cytotoxic agents. In this review, we briefly discuss the potential molecular targets, and the challenges of targeted brain tumor treatment. For example, glial tumors are associated with over-expression of calcium-dependent potassium (KCa) channels, and high grade glioma express specific KCa channel gene (gBK) splice variants, and mutant epidermal growth factor receptors (EGFRvIII). These specific genes are promising targets for molecular targeted treatment in brain tumors. In addition, drugs like Avastin and Gleevec target the molecular targets such as vascular endothelial cell growth factor receptor, platelet-derived growth factor receptors, and BRC-ABL/Akt. Recent discovery of non-coding RNA, specifically microRNAs could be used as potential targeted drugs. Finally, we discuss the role of anti-cancer drug delivery to brain tumors by breaching the blood-brain tumor barrier. This non-invasive strategy is particularly useful as novel molecules and humanized monoclonal antibodies that target receptor tyrosine kinase receptors are rapidly being developed.
机译:脑肿瘤与预后不良有关。尽管在理解脑肿瘤的病因学和分子生物学方面取得了巨大进步,这已导致开发药物策略和正在进行的NCI / Pharma赞助的临床试验取得了突破,但对于脑肿瘤患者而言,治疗选择仍然受到严格限制。我们回顾了过去十年来在脑肿瘤的临床前和临床研究中有关分子靶向药物的文献,并观察到脑肿瘤中的分子靶向是复杂的。这是因为单个分子试剂不会影响单个基因或蛋白质,因此需要将分子疗法与细胞毒剂联合使用。在这篇综述中,我们简要讨论了潜在的分子靶标以及靶向脑肿瘤治疗的挑战。例如,神经胶质瘤与钙依赖性钾(KCa)通道的过表达有关,高级神经胶质瘤表达特定的KCa通道基因(gBK)剪接变体和突变表皮生长因子受体(EGFRvIII)。这些特异性基因是脑肿瘤分子靶向治疗的有希望的靶标。此外,像Avastin和Gleevec这样的药物靶向分子靶标,例如血管内皮细胞生长因子受体,血小板衍生的生长因子受体和BRC-ABL / Akt。非编码RNA,特别是微RNA的最新发现可以用作潜在的靶向药物。最后,我们讨论了通过突破血脑肿瘤屏障来将抗癌药物递送至脑肿瘤的作用。随着新型分子的发展以及靶向受体酪氨酸激酶受体的人源化单克隆抗体的快速开发,这种非侵入性策略特别有用。

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