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首页> 外文期刊>Journal of Korean Neurosurgical Society >Clinical Pearls and Advances in Molecular Researches of Epilepsy-Associated Tumors
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Clinical Pearls and Advances in Molecular Researches of Epilepsy-Associated Tumors

机译:癫痫相关肿瘤的分子生物学研究与临床进展

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摘要

Brain tumors are the second most common type of structural brain lesion that causes chronic epilepsy. Patients with low-grade brain tumors often experience chronic drug-resistant epilepsy starting in childhood, which led to the concept of long-term epilepsy-associated tumors (LEATs). Dysembryoplastic neuroepithelial tumor and ganglioglioma are representative LEATs and are characterized by young age of onset, frequent temporal lobe location, benign tumor biology, and chronic epilepsy. Although highly relevant in clinical epileptology, the concept of LEATs has been criticized in the neuro-oncology field. Recent genomic and molecular studies have challenged traditional views on LEATs and low-grade gliomas. Molecular studies have revealed that low-grade gliomas can largely be divided into three groups : LEATs, pediatric-type diffuse low-grade glioma (DLGG; astrocytoma and oligodendroglioma), and adult-type DLGG. There is substantial overlap between conventional LEATs and pediatric-type DLGG in regard to clinical features, histology, and molecular characteristics. LEATs and pediatric-type DLGG are characterized by mutations in BRAF, FGFR1, and MYB/MYBL1, which converge on the RAS-RAF-MAPK pathway. Gene (mutation)-centered classification of epilepsy-associated tumors could provide new insight into these heterogeneous and diverse neoplasms and may lead to novel molecular targeted therapies for epilepsy in the near future.
机译:脑肿瘤是导致慢性癫痫的第二种最常见的结构性脑部病变。患有低度脑肿瘤的患者通常从儿童时期开始经历慢性耐药性癫痫病,这导致了长期癫痫相关肿瘤(LEATs)的概念。发育不良的神经上皮肿瘤和神经节神经胶质瘤是典型的LEATs,其特征是发病年龄小,颞叶位置频繁,肿瘤良性生物学和慢性癫痫。尽管在临床癫痫学中高度相关,但LEATs的概念已在神经肿瘤学领域受到批评。最近的基因组和分子研究挑战了有关LEATs和低级神经胶质瘤的传统观点。分子研究表明,低级神经胶质瘤可大致分为三类:LEATs,小儿型弥漫性低级神经胶质瘤(DLGG;星形细胞瘤和少突胶质细胞瘤)和成人型DLGG。就临床特征,组织学和分子特征而言,传统的LEAT和小儿型DLGG之间存在很大的重叠。 LEAT和小儿型DLGG的特征是BRAF,FGFR1和MYB / MYBL1中的突变,它们会收敛于RAS-RAF-MAPK途径。以基因(突变)为中心的癫痫相关肿瘤分类可以为这些异质性和多样化肿瘤提供新的见识,并可能在不久的将来导致新的针对癫痫的分子靶向疗法。

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