Rath Barbara, Plangger Adelina, Hamilton Gerhard
Department of Vascular Surgery, Medical University of Vienna, Vienna A-1090, Austria.
Cancer Drug Resist. 2020 Feb 28;3(2):171-178. doi: 10.20517/cdr.2019.85. eCollection 2020.
Mutated or rearranged driver kinases in non-small cell lung cancer (NSCLC) cells are clinically amenable to treatment with tyrosine kinase inhibitors (TKIs) resulting in prolonged survival and significant benefit compared to cytotoxic chemotherapy. The most frequent genomic alterations are observed for epidermal growth factor receptor and anaplastic lymphoma kinase, which can be blocked by a range of specific TKIs in sequence. In clinics, resistance to TKIs emerges after approximately one year and comprises secondary mutations of the kinases (on-target) or alternative pathways circumventing the original kinase (off-target) alterations. A special feature of NSCLC is the occurrence of histological transformation to small cell lung cancer (SCLC) in up to 14% of cases, which, in general, is accompanied by resistance to the original TKIs. SCLC transformed tumors may be treated with the classical platinum/etoposide regimen but thus far there are no definitive guidelines. Four transformed pleural SCLC lines in our lab indicate the presence of a gradual NSCLC-SCLC shift with overlapping drug sensitivities. In conclusion, the treatment of NSCLC-SCLC transformed cancer cells would need a better chemosensitivity assessment using functional genomics to guide further therapy.
非小细胞肺癌(NSCLC)细胞中发生突变或重排的驱动激酶在临床上适合用酪氨酸激酶抑制剂(TKIs)进行治疗,与细胞毒性化疗相比,可延长生存期并带来显著益处。最常见的基因组改变见于表皮生长因子受体和间变性淋巴瘤激酶,它们可被一系列特定的TKIs依次阻断。在临床上,对TKIs的耐药性大约在一年后出现,包括激酶的二次突变(靶向)或绕过原始激酶的替代途径(非靶向)改变。NSCLC的一个特殊特征是在高达14%的病例中会发生组织学转化为小细胞肺癌(SCLC),一般来说,这伴随着对原始TKIs的耐药性。转化为SCLC的肿瘤可用经典的铂/依托泊苷方案治疗,但迄今为止尚无明确的指南。我们实验室的四个转化的胸膜SCLC细胞系表明存在逐渐的NSCLC - SCLC转变以及重叠的药物敏感性。总之,NSCLC - SCLC转化癌细胞的治疗需要使用功能基因组学进行更好的化学敏感性评估,以指导进一步治疗。
