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Molecular characterization of head and neck cancer: How close to personalized targeted therapy?

机译:头颈癌的分子特征:与个性化靶向治疗有多接近?

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Molecular targeted therapy in head and neck squamous cell carcinoma (HNSCC) continues to make strides, and holds much promise. Cetuximab remains the sole US FDA-approved molecular targeted therapy available for HNSCC, though several new biologic agents targeting the epidermal growth factor receptor (EGFR) and other pathways are currently in the regulatory approval pipeline. While targeted therapies have the potential to be personalized, their current use in HNSCC is not personalized. This is illustrated for EGFR-targeted drugs, where EGFR as a molecular target has yet to be individualized for HNSCC. Future research needs to identify factors that correlate with response (or lack of one) and the underlying genotype-phenotype relationship that dictates this response. Comprehensive exploration of genetic and epigenetic landscapes in HNSCC is opening new frontiers to further enlighten and mechanistically inform newer as well as existing molecular targets, and to set a course for eventually translating these discoveries into therapies for patients. This opinion offers a snapshot of the evolution of molecular subtyping in HNSCC and its current clinical applicability, as well as new emergent paradigms with implications for controlling this disease in the future.
机译:头颈部鳞状细胞癌(HNSCC)的分子靶向治疗继续取得长足进步,并具有很大的前景。西妥昔单抗仍然是美国FDA批准的可用于HNSCC的唯一分子靶向疗法,尽管目前有数种针对表皮生长因子受体(EGFR)和其他途径的新型生物制剂正在监管审批中。尽管靶向疗法具有个性化的潜力,但它们在HNSCC中的当前使用尚未个性化。 EGFR靶向药物对此进行了说明,其中EGFR作为分子靶标尚未针对HNSCC进行个性化处理。未来的研究需要确定与反应(或缺乏反应)相关的因素以及决定该反应的潜在基因型与表型关系。对HNSCC的遗传和表观遗传学景观的全面探索为开拓新领域开辟了新的领域,以进一步启迪并以机械方式为新近和现有的分子靶标提供信息,并为最终将这些发现转化为患者的治疗方法奠定了基础。该观点为HNSCC分子亚型的演变及其当前的临床适用性提供了快照,并提供了可能在将来控制这种疾病的新出现的范例。

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