Spotlight on brigatinib and its potential in the treatment of patients with metastatic ALK-positive non-small cell lung cancer who are resistant or intolerant to crizotinib.

IF 5.1 Q1 ONCOLOGY Lung Cancer: Targets and Therapy Pub Date : 2017-10-13 eCollection Date: 2017-01-01 DOI:10.2147/LCTT.S126507
Rohit K Jain, Hongbin Chen
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Abstract

In the last decade, there have been major therapeutic advances in the management of patients with anaplastic lymphoma kinase (ALK)-positive non-small cell lung cancer. Crizotinib was the first approved ALK inhibitor with significant benefits over chemotherapy. However, patients inevitably develop disease progression especially in central nervous system and acquire resistance to crizotinib. Several next-generation ALK inhibitors have been developed to overcome these resistance mechanisms and have demonstrated clinical benefits in crizotinib-refractory non-small cell lung cancer including in central nervous system. Brigatinib is a second-generation ALK inhibitor with high level of activity against ALK and several other targets. It is active in vitro against many ALK kinase domain mutations including L1196M, E1210K, and G1202R which may mediate acquired resistance to other ALK inhibitors. In Phase I/II and ALTA clinical studies, brigatinib has demonstrated substantial and durable responses and intracranial responses after progression on crizotinib. It has acceptable safety profile, but early pulmonary toxicity has been observed prompting to pursue daily dosing of 180 mg (with lead-in). Overall, 180 mg (with lead-in) has showed consistently better efficacy than 90 mg. In this review, we will discuss in detail these two pivotal trials that led to the accelerated approval for brigatinib and its future directions.

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聚焦布加替尼及其在治疗对克唑替尼耐药或不耐受的转移性ALK阳性非小细胞肺癌患者方面的潜力。
近十年来,无性淋巴瘤激酶(ALK)阳性非小细胞肺癌患者的治疗取得了重大进展。克唑替尼是首个获批的 ALK 抑制剂,与化疗相比疗效显著。然而,患者不可避免地会出现疾病进展,尤其是中枢神经系统,并对克唑替尼产生耐药性。为了克服这些耐药机制,目前已开发出几种新一代 ALK 抑制剂,并已在克唑替尼难治性非小细胞肺癌(包括中枢神经系统)中显示出临床疗效。Brigatinib 是第二代 ALK 抑制剂,对 ALK 和其他几个靶点具有很高的活性。它对许多 ALK 激酶域突变具有体外活性,包括 L1196M、E1210K 和 G1202R,这些突变可能介导对其他 ALK 抑制剂的获得性耐药性。在I/II期和ALTA临床研究中,布加替尼显示出了显著而持久的应答,并在克唑替尼治疗进展后出现了颅内应答。它的安全性可以接受,但观察到了早期肺部毒性,这促使它继续采用每天 180 毫克(含前导药)的剂量。总体而言,180 毫克(含前导药)的疗效一直优于 90 毫克。在本综述中,我们将详细讨论这两项促使布加替尼加速获批的关键试验及其未来发展方向。
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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
期刊最新文献
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