Overcoming MET-Dependent Resistance to Selective RET Inhibition in Patients with RET Fusion–Positive Lung Cancer by Combining Selpercatinib with Crizotinib

克里唑蒂尼 医学 肺癌 癌症研究 卡波扎尼布 融合基因 间变性淋巴瘤激酶 ROS1型 酪氨酸激酶 靶向治疗 癌症 碱性抑制剂 受体酪氨酸激酶 甲状腺髓样癌 酪氨酸激酶抑制剂 内科学 肿瘤科 腺癌 甲状腺癌 生物 基因 受体 遗传学 恶性胸腔积液
作者
Ezra Y. Rosen,Melissa L. Johnson,Sarah Clifford,Romel Somwar,Jennifer Kherani,Jieun Son,Arrien A. Bertram,Monika A. Davare,Eric Gladstone,Elena V. Ivanova,Dahlia N. Henry,Elaine M. Kelley,Mika Lin,Marina S.D. Milan,Binoj C. Nair,Elizabeth Olek,Jenna E. Scanlon,Morana Vojnic,Kevin Ebata,Jaclyn F. Hechtman
出处
期刊:Clinical Cancer Research [American Association for Cancer Research]
卷期号:27 (1): 34-42 被引量:123
标识
DOI:10.1158/1078-0432.ccr-20-2278
摘要

Abstract Purpose: The RET proto-oncogene encodes a receptor tyrosine kinase that is activated by gene fusion in 1%–2% of non–small cell lung cancers (NSCLC) and rarely in other cancer types. Selpercatinib is a highly selective RET kinase inhibitor that has recently been approved by the FDA in lung and thyroid cancers with activating RET gene fusions and mutations. Molecular mechanisms of acquired resistance to selpercatinib are poorly understood. Patients and Methods: We studied patients treated on the first-in-human clinical trial of selpercatinib (NCT03157129) who were found to have MET amplification associated with resistance to selpercatinib. We validated MET activation as a targetable mediator of resistance to RET-directed therapy, and combined selpercatinib with the MET/ALK/ROS1 inhibitor crizotinib in a series of single patient protocols (SPP). Results: MET amplification was identified in posttreatment biopsies in 4 patients with RET fusion–positive NSCLC treated with selpercatinib. In at least one case, MET amplification was clearly evident prior to therapy with selpercatinib. We demonstrate that increased MET expression in RET fusion–positive tumor cells causes resistance to selpercatinib, and this can be overcome by combining selpercatinib with crizotinib. Using SPPs, selpercatinib with crizotinib were given together generating anecdotal evidence of clinical activity and tolerability, with one response lasting 10 months. Conclusions: Through the use of SPPs, we were able to offer combination therapy targeting MET-amplified resistance identified on the first-in-human study of selpercatinib. These data suggest that MET dependence is a recurring and potentially targetable mechanism of resistance to selective RET inhibition in advanced NSCLC.
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