Sotorasib (AMG 510)治疗KRAS G12C阳性非小细胞肺癌

IF 5.1 Q1 ONCOLOGY
Lung Cancer: Targets and Therapy Pub Date : 2021-10-07 eCollection Date: 2021-01-01 DOI:10.2147/LCTT.S334623
Shannon S Zhang, Misako Nagasaka
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引用次数: 13

摘要

KRAS密码子12突变已在13%的非小细胞肺癌患者中被发现。开发针对KRASG12C突变的靶向治疗已被证明是具有挑战性的,因为细胞质中有丰富的GTP, GTP的快速水解,以及难以设计小分子以达到足够的浓度来抑制KRAS。基于临床前和临床试验的良好结果,新型KRASG12C抑制剂sotorasib于2021年5月获得FDA的有条件批准。临床试验的I期部分产生了32%的确诊反应,56%的患者病情稳定。接受每日最高剂量960mg的患者中,约91.2%的患者实现了疾病控制。II期部分,使用每日960mg剂量,导致37.1%的患者确认缓解,80.6%的患者疾病控制。I期和II期的无进展生存期相似,分别为6.3个月和6.8个月。在这两个阶段中,4级不良事件仅发生在一名患者中。最常见的不良事件是LFTs升高,在剂量减少和类固醇治疗后呈下降趋势。虽然sotorasib的有条件批准对那些携带KRASG12C突变的患者来说是一个重大突破,但对sotorasib的耐药突变越来越普遍。为解决这一问题,已经提出了许多建议,例如使用联合疗法治疗合成致死率,这些建议正在产生令人鼓舞的结果。在这里,我们进一步详细探讨了sotorasib的发展,其功效,耐药机制,以及克服这些耐药的策略。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Spotlight on Sotorasib (AMG 510) for <i>KRAS</i> <sup>G12C</sup> Positive Non-Small Cell Lung Cancer.

Spotlight on Sotorasib (AMG 510) for <i>KRAS</i> <sup>G12C</sup> Positive Non-Small Cell Lung Cancer.

Spotlight on Sotorasib (AMG 510) for KRAS G12C Positive Non-Small Cell Lung Cancer.

Mutations in codon 12 of KRAS have been identified in 13% of non-small cell lung cancer patients. Developing targeted therapies against KRASG12C mutation has proven to be challenging due to the abundance of GTP in the cytoplasm, rapid hydrolysis of GTP, and difficulty designing small molecules to achieve sufficient concentration for KRAS inhibition. Based on promising results in both preclinical and clinical trials, sotorasib, a novel KRASG12C inhibitor, was given conditional approval by the FDA in May 2021. The Phase I portion of the clinical trial produced 32% confirmed response with 56% of patients with stable disease. About 91.2% of patients who received the highest dose of 960mg daily achieved disease control. The Phase II portion, which used 960mg daily dosing resulted in 37.1% of patients with confirmed response and 80.6% of patients with disease control. Both phase I and phase II had similar progression-free survival, in 6.3 months and 6.8 months, respectively. In both phases, grade 4 adverse events occurred in only one patient. The most common adverse events were elevations in LFTs, which down-trended upon dose reduction and steroid treatment. While the conditional approval of sotorasib was a major breakthrough for those patients harboring KRASG12C mutations, resistance mutations to sotorasib are increasingly common. Many proposals have been made to address this, such as the use of combination therapy for synthetic lethality, which are producing encouraging results. Here, we explore in further detail the development of sotorasib, its efficacy, mechanism of resistance, and strategies to overcome these resistances.

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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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