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黑色素瘤脑转移的当前治疗方法。

Current Treatment of Melanoma Brain Metastasis.

机构信息

Department of Radiation Oncology, H. Lee Moffitt Cancer Center and Research Institute, 12902 USF Magnolia Dr, Tampa, FL, 33612, USA.

出版信息

Curr Treat Options Oncol. 2020 Apr 30;21(6):45. doi: 10.1007/s11864-020-00733-z.

Abstract

With greater understanding of underlying biology and development of effective BRAF-targeted therapy and immunotherapy, along with remarkable advances in local treatment such as stereotactic radiosurgery, melanoma brain metastasis (MBM) is witnessing continually improving outcome, with 1-year overall survival rate approaching 85%. Given disease complexity and myriad treatment options, all patients with MBM should ideally be evaluated in a multidisciplinary setting to allow an individualized treatment approach based on prognostic groups, molecular classification, number and size of brain metastasis, and performance status. With improving outcome, pendulum has now swayed to focus more on effective treatment modalities with minimal neurological toxicity while maintaining quality of life. Surgery is usually considered in symptomatic and large MBMs, while stereotactic radiosurgery considered in 1-4 lesions, and now also being explored for up to 15 brain metastases for improved local control. The role of whole brain radiotherapy is diminishing given its neurocognitive toxicities and is reserved for patients with diffuse brain involvement. Cytotoxic chemotherapy has largely been ineffective without evidence for survival benefit. Immune checkpoint inhibitors have become the cornerstone of management for melanoma brain metastasis with durable intracranial tumor control and excellent toxicity profile. For patients with asymptomatic MBMs, ipilimumab and nivolumab have shown intracranial response near 60% and provides comparable clinical benefit in MBMs as for extracranial metastases. For patients with driver BRAF mutation, BRAFi-/MEKi-targeted agents are proven to be effective in MBM with high rate intracranial responses (44-59%). However, the durability of intracranial responses induced by BRAFi/MEKi seems to be shorter than that of extracranial disease. Emerging data support novel combination of systemic therapy and stereotactic radiosurgery, which appears to be safe and effective; however, potential benefits and risks should be evaluated prospectively. Promising ongoing trials will further expand therapeutic evidence in MBM, and patients should be encouraged to participate in clinical trials.

摘要

随着对潜在生物学机制的深入了解,以及针对 BRAF 的有效靶向治疗和免疫疗法的发展,加上立体定向放射外科等局部治疗手段的显著进步,黑色素瘤脑转移(MBM)的治疗效果不断改善,1 年总生存率接近 85%。鉴于疾病的复杂性和众多治疗选择,所有 MBM 患者都应在多学科环境中进行评估,以便根据预后分组、分子分类、脑转移数量和大小以及身体状况,制定个体化的治疗方法。随着治疗效果的提高,现在的重点更多地放在了具有最小神经毒性的有效治疗方式上,同时保持生活质量。手术通常适用于有症状和大的 MBM,而立体定向放射外科适用于 1-4 个病灶,现在也在探索用于多达 15 个脑转移灶,以提高局部控制率。全脑放疗的作用因神经认知毒性而减弱,仅适用于弥漫性脑受累的患者。细胞毒性化疗的效果不佳,没有生存获益的证据。免疫检查点抑制剂已成为 MBM 治疗的基石,可实现持久的颅内肿瘤控制和良好的毒性特征。对于无症状的 MBM 患者,伊匹单抗和纳武单抗显示出近 60%的颅内缓解率,并为 MBM 患者提供了与颅外转移相当的临床获益。对于携带驱动 BRAF 突变的患者,BRAFi/MEKi 靶向药物在 MBM 中显示出有效的颅内反应率(44-59%)。然而,与颅外疾病相比,BRAFi/MEKi 诱导的颅内反应的持久性似乎更短。新的系统治疗和立体定向放射外科联合治疗的疗效和安全性数据支持这一方法,但应前瞻性评估潜在的获益和风险。有前景的正在进行的临床试验将进一步扩大 MBM 的治疗证据,应鼓励患者参与临床试验。

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