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首页> 外文期刊>The oncologist >Emerging Gene Fusion Drivers in Primary and Metastatic Central Nervous System Malignancies: A Review of Available Evidence for Systemic Targeted Therapies
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Emerging Gene Fusion Drivers in Primary and Metastatic Central Nervous System Malignancies: A Review of Available Evidence for Systemic Targeted Therapies

机译:在原发性和转移性中枢神经系统恶性肿瘤中的新兴基因融合驱动程序:系统靶向治疗的可用证据综述。

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Primary and metastatic tumors of the central nervous system present a difficult clinical challenge, and they are a common cause of disease progression and death. For most patients, treatment consists primarily of surgery and/or radiotherapy. In recent years, systemic therapies have become available or are under investigation for patients whose tumors are driven by specific genetic alterations, and some of these targeted treatments have been associated with dramatic improvements in extracranial and intracranial disease control and survival. However, the success of other systemic therapies has been hindered by inadequate penetration of the drug into the brain parenchyma. Advances in molecular characterization of oncogenic drivers have led to the identification of new gene fusions driving oncogenesis in some of the most common sources of intracranial tumors. Systemic therapies targeting many of these alterations have been approved recently or are in clinical development, and the ability to penetrate the blooda??brain barrier is now widely recognized as an important property of such drugs. We review this rapidly advancing field with a focus on recently uncovered gene fusions and braina??penetrant systemic therapies targeting them. Implications for Practice. Driver gene fusions involving receptor tyrosine kinases have been identified across a wide range of tumor types, including primary central nervous system (CNS) tumors and extracranial solid tumors that are associated with high rates of metastasis to the CNS (e.g., lung, breast, melanoma). This review discusses the systemic therapies that target emerging gene fusions, with a focus on braina??penetrant agents that will target the intracranial disease and, where present, also extracranial disease.
机译:中枢神经系统的原发性和转移性肿瘤提出了困难的临床挑战,并且它们是疾病进展和死亡的常见原因。对于大多数患者,治疗主要包括手术和/或放射疗法。近年来,对于由特定遗传改变驱动肿瘤的患者,已经可以使用全身疗法或正在研究全身疗法,并且其中一些靶向疗法与颅外和颅内疾病控制和生存的显着改善相关。但是,其他全身疗法的成功已因药物无法充分渗透到脑实质中而受到阻碍。致癌驱动因子的分子表征研究进展已导致鉴定出一些在颅内肿瘤的最常见来源中驱动致癌作用的新基因融合体。针对许多这些改变的全身疗法最近已经被批准或正在临床开发中,并且渗透血脑屏障的能力现已被广泛认为是这类药物的重要特性。我们回顾了这个迅速发展的领域,重点是最近发现的基因融合和针对它们的脑部渗透性全身疗法。对实践的启示。已在多种肿瘤类型中鉴定出涉及受体酪氨酸激酶的驱动基因融合体,包括原发性中枢神经系统(CNS)肿瘤和与CNS高转移率相关的颅外实体瘤(例如,肺,乳腺,黑色素瘤) )。这篇综述讨论了针对新兴基因融合的系统疗法,重点是针对颅内疾病以及颅外疾病的脑通透剂。

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