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Current management of low-grade gliomas.

机译:目前对低度神经胶质瘤的治疗。

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摘要

PURPOSE OF REVIEW: The management of patients suffering from low-grade gliomas (LGGs) remains a challenge in absence of a definite curative therapy. The median survival is highly variable, from 2 years (high-risk disease) to over 15 years (low risk). The aim of this review is to provide a practical step-by-step evaluation of the available treatment options for patients with LGGs.RECENT FINDINGS: Next to clinical prognostic markers, both the isocitrate dehydrogenase (IDH) mutation status and the status of 1p/19q codeletion are key prognostic factors for the optimal management of patients with LGG. Two recent randomized phase III clinical trials were performed in LGGs. They first compared the efficacy of radiation versus temozolomide (TMZ) chemotherapy in high-risk LGGs. The second trial compared radiation versus radiation combined with procarbazine, lomustine and vincristine chemotherapy.SUMMARY: Regarding molecular prognostic factors, IDH wild-type LGGs have the worst prognosis, independent of therapy, whereas patients with mutated IDH, codeleted 1p/19q LGGs fared best regarding progression-free survival (PFS). In high-risk LGGs, PFS is similar regardless of whether patients have been treated with radiation or TMZ. In the second trial, patients who were treated with combination radiation and chemotherapy showed significant longer overall survival.
机译:审查的目的:在缺乏明确的治疗方法的情况下,低度神经胶质瘤(LGGs)患者的治疗仍然是一个挑战。中位生存期变化很大,从2年(高危疾病)到15年以上(低危)。这篇综述的目的是为LGG患者的可用治疗方案提供切实可行的逐步评估。最新发现:除了临床预后指标外,异柠檬酸脱氢酶(IDH)突变状态和1p / 19q编码是LGG患者最佳治疗的关键预后因素。 LGG中进行了两项近期的随机III期临床试验。他们首先比较了放疗与替莫唑胺(TMZ)化疗在高危LGG中的疗效。第二项试验比较了放疗与放疗联合丙卡巴嗪,洛莫斯汀和长春新碱的放疗。总结:关于分子预后因素,IDH野生型LGGs的预后最差,与治疗无关,而IDH突变的IDp为1p / 19q LGGs的患者预后最好。关于无进展生存期(PFS)。在高危LGG中,无论是否接受放射线治疗或TMZ治疗,PFS都是相似的。在第二项试验中,接受放射线和化学疗法联合治疗的患者显示出更长的总生存期。

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