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New therapeutic options in systemic treatment of advanced cutaneous melanoma

机译:系统性治疗晚期皮肤黑色素瘤的新疗法

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Introduction: For many years systemic treatment of advanced/metastatic melanoma has been based on chemotherapy or immunotherapy. However, even very toxic regimens (e.g., polychemotherapy, bio-chemotherapy or immunotherapy with HD-IL-2) despite increased response rates as compared with standard dacarbazine monotherapy have not improved patients' outcomes. Over the last two decades, a huge effort, made in order to determine the molecular and immunological mechanisms responsible for biology of melanoma led to development of novel targeted agents. Areas covered: The aim of this article is to summarize data on novel targeted agents used for treatment of metastatic melanoma. The authors searched PubMed, EMBASE and abstracts from ASCO, ESMO, AACR congresses for Phase II/III clinical studies evaluating novel immunomodulating agents and kinase inhibitors in melanoma patients. Expert opinion: Elucidation of the crucial role of MAPK pathway and BRAF kinase mutations in particular has led to development of specific small molecule kinase inhibitors (vemurafenib, dabrafenib, trametinib), and new insight into molecular mechanisms responsible for immune response and tolerance resulted in development of immunomodulatory agents (ipilimumab, anti-PD1, anti-PD-L1). The introduction of novel drugs has changed the natural history of melanoma. However, it has also generated new clinical challenges that have to be resolved as soon as possible.
机译:简介:多年来,对晚期/转移性黑色素瘤的全身治疗一直基于化学疗法或免疫疗法。然而,尽管与标准达卡巴嗪单药疗法相比,尽管反应率提高,但即使是毒性很大的疗法(例如,多化学疗法,生物化学疗法或HD-IL-2免疫疗法)也无法改善患者的预后。在过去的二十年中,为了确定负责黑色素瘤生物学的分子和免疫学机制而付出的巨大努力导致了新型靶向药物的开发。涵盖的领域:本文的目的是总结用于治疗转移性黑色素瘤的新型靶向药物的数据。作者在PubMed,EMBASE和ASCO,ESMO,AACR大会摘要中进行搜索,以进行II / III期临床研究,评估黑色素瘤患者的新型免疫调节剂和激酶抑制剂。专家意见:阐明MAPK途径和BRAF激酶突变的关键作用尤其导致了特定小分子激酶抑制剂(vemurafenib,dabrafenib,trametinib)的发展,并且对负责免疫应答和耐受的分子机制有了新的认识免疫调节剂(ipilimumab,抗PD1,抗PD-L1)的检测。新药的引入改变了黑素瘤的自然史。但是,它也产生了新的临床挑战,必须尽快解决。

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