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异柠檬酸脱氢酶(IDH)突变型神经胶质瘤治疗进展:IDH抑制剂、INDIGO试验的临床意义及未来展望

Advances in IDH-mutant glioma management: IDH inhibitors, clinical implications of INDIGO trial, and future perspectives.

作者信息

Mojica Christianne V, Gutierrez Katrina Mari E, Mason Warren P

机构信息

Divisions of Neurology and Medical Oncology and Hematology, Princess Margaret Cancer Centre, University Health Network, Toronto, Ontario, Canada.

出版信息

Future Oncol. 2025 Jul;21(16):2089-2099. doi: 10.1080/14796694.2025.2511587. Epub 2025 May 27.

Abstract

The discovery of isocitrate dehydrogenase (IDH) mutation in gliomas marked the new era of molecular classification of CNS tumors. Understanding the complex role of IDH mutation in oncogenesis led to the evaluation of novel small molecules targeting this enzyme as a potential therapeutic intervention. Vorasidenib, a brain-penetrant inhibitor of both IDH1 and IDH2-mutant enzymes, was one such agent. The phase 3 INDIGO trial evaluated vorasidenib and demonstrated its efficacy in IDH-mutant low-grade gliomas (LGG). This study established vorasidenib as an effective inhibitor of both IDH1 and IDH2-mutant enzymes, highlighting its great potential in advancing the therapeutic armamentarium for patients with LGG. While vorasidenib has been recently included in several treatment guidelines for CNS tumors, further research on the use of this novel agent, as monotherapy or in combination with other drugs, becomes imperative to exploit fully its potential in the management of IDH-mutant gliomas.

摘要

胶质瘤中异柠檬酸脱氢酶(IDH)突变的发现标志着中枢神经系统肿瘤分子分类的新时代。了解IDH突变在肿瘤发生中的复杂作用促使人们评估靶向该酶的新型小分子作为一种潜在的治疗干预措施。伏立西尼(Vorasidenib)就是这样一种药物,它是一种可穿透血脑屏障的IDH1和IDH2突变酶抑制剂。3期INDIGO试验对伏立西尼进行了评估,并证明了其在IDH突变型低级别胶质瘤(LGG)中的疗效。这项研究确立了伏立西尼作为IDH1和IDH2突变酶的有效抑制剂,突出了其在推进LGG患者治疗手段方面的巨大潜力。虽然伏立西尼最近已被纳入多项中枢神经系统肿瘤治疗指南,但对这种新型药物作为单一疗法或与其他药物联合使用的进一步研究势在必行,以便充分发挥其在IDH突变型胶质瘤治疗中的潜力。

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Vorasidenib in IDH1- or IDH2-Mutant Low-Grade Glioma.沃拉西尼布治疗 IDH1 或 IDH2 突变型低级别胶质瘤。
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本文引用的文献

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Treatment of IDH-mutant glioma in the INDIGO era.INDIGO时代IDH突变型胶质瘤的治疗
NPJ Precis Oncol. 2024 Jul 19;8(1):149. doi: 10.1038/s41698-024-00646-2.

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