在 Cemiplimab NSCLC FDA 适应症(EMPOWER-肺 1 和-肺 3)中额外排除 ROS1 融合(除 EGFR 突变和 ALK 融合外)。了解免疫疗法在以不吸烟者为主的可作用驱动基因突变阳性 NSCLC 中的当前科学前景?

IF 5.1 Q1 ONCOLOGY Lung Cancer: Targets and Therapy Pub Date : 2023-06-23 eCollection Date: 2023-01-01 DOI:10.2147/LCTT.S413611
Danielle Brazel, Saihong Ignatius Ou
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引用次数: 0

摘要

根据 EMPOWER-Lung 1 和 -Lung 3 试验,Cemiplimab 是美国批准用于晚期 NSCLC 一线(1L)治疗的七种免疫检查点抑制剂(ICIs)之一。除了排除表皮生长因子受体(EGFR)突变和 ALK 融合的 NSCLC 患者接受 ICIs 的 1L 治疗外,根据 EMPOWER 肺部试验的设计,排除 ROS1 融合是美国 FDA 适应症中使用 cemiplimab 的另一个独特的排除标准。我们回顾了 ICIs 对具有驱动基因突变(表皮生长因子受体、ALK、ROS1、RET、HER2)的从不吸烟者为主的 NSCLC 的有效性,并质疑排除 ROS1 融合是否会使 cemiplimab 在竞争中处于劣势,因为保险要求证明 ROS1 融合阴性。我们进一步讨论了美国 FDA 作为监管机构是否有权利和责任协调 ICIs 在这些可操作的驱动基因突变中的使用,以规范社区实践,造福患者,并推动针对这些驱动基因突变的新一代治疗方法的开发。
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The Additional Exclusions of ROS1 Fusions (In Addition to EGFR Mutation and ALK Fusions) in the Cemiplimab NSCLC FDA Indication (EMPOWER-Lung 1 and -Lung 3). Catching Up with Current Scientific View of Immunotherapy in Never-Smoker Predominant Actionable Driver Mutation Positive NSCLC?

Cemiplimab is one of seven immune checkpoint inhibitors (ICIs) approved for the first-line (1L) treatment of advanced NSCLC in the US based on EMPOWER-Lung 1 and -Lung 3 trials. In addition to exclusion of NSCLC patients harboring EGFR mutations and ALK fusion from 1L treatment with ICIs, exclusion of ROS1 fusion is an additional unique exclusion the use of criterion for cemiplimab in the US FDA indication based on the design of the EMPOWER lung trials. We review the effectiveness of ICIs in never-smoker predominant NSCLC with driver mutations (EGFR, ALK, ROS1, RET, HER2) and question whether exclusion of ROS1 fusion would put cemiplimab at a competitive disadvantage given the requirement for insurance to prove ROS1 fusion negativity. We further discuss whether the US FDA as a regulatory authority has the right and responsibility to harmonize the use of ICIs in these actionable driver mutations to standardize community practice for the benefit of patients and to advance the development of next-generation treatment for these driver mutations.

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来源期刊
CiteScore
8.10
自引率
0.00%
发文量
10
审稿时长
16 weeks
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