Piechocki Marie P, Yoo George H, Dibbley Susan K, Lonardo Fulvio
Department of Otolaryngology-Head and Neck Surgery, Wayne State University, 110 East Warren Avenue, Detroit, MI 48201, USA.
Cancer Res. 2007 Jul 15;67(14):6825-43. doi: 10.1158/0008-5472.CAN-07-0765.
The HER2/neu oncogene is an important diagnostic and prognostic factor and therapeutic target in breast and other cancers. We developed and characterized a breast cancer cell line (Bam1a) that overexpresses the activated HER2/neu and ErbB-3 and has a gene expression profile consistent with the ErbB-2 genetic signature. We evaluated the effects of the epidermal growth factor receptor (EGFR)/HER2 inhibitor, gefitinib, on this breast tumor line in vitro and in vivo. We characterized the effects of gefitinib on EGFR, HER2, and ErbB-3 phosphorylation by Western blot and determined the effects on downstream signaling through growth, survival, and stress pathways and the effect on proliferation, cell cycle, and apoptosis. Gefitinib treatment diminished phosphorylation of the ErbB-3 > EGFR > HER2/neu and signal transducers and activators of transcriptions in a dose-dependent fashion. Downstream mitogenic signaling through mitogen-activated protein (MAP)/extracellular signal regulated kinase kinase, p44/42 MAP kinase (MAPK) and stress signaling through c-Jun-NH(2)-kinase (JNK) 1 and c-Jun was impaired (1 micromol/L, 4-24 h), leading to cytostasis and cell cycle arrest within 24 h by decreased cyclin D1, cyclin B1, and p(Ser795)Rb and increased p27. Proliferation and colony formation were inhibited at 0.5 and 1 micromol/L, respectively, and correlated with altered gene expression profiles. Diminished survival signaling through Akt, induction of bim, loss of connexin43, and decreased production of vascular endothelial growth factor-D preceded caspase-3 and poly(ADP)ribose polymerase (PARP) cleavage and apoptosis (>50% 2 micromol/L, 48 h). Oral administration of gefitinib was able to prevent the outgrowth of Bam1a tumor cells from palpable lesions, shrink established tumors, eliminate HER2 and HER3 phosphorylation, and decrease MAPK and Akt signaling in vivo. A variant of the Bam1a cell line, IR-5, with acquired ability to grow in 5 micromol/L gefitinib was developed and characterized. IR-5 bears a novel point mutation in the HER2/neu that corresponds to a L726I in the ATP-binding pocket and correlates with a log decrease in sensitivity to gefitinib, increased heterodimerization with EGFR and HER3, and impaired down-regulation. Gene expression profiling of IR-5 showed increased expression of EMP-1, NOTCH-1, FLT-1, PDGFB, and several other genes that may contribute to the resistant phenotype and sustain signaling through MAPK and Akt. This model will be useful in understanding the differences between intrinsic drug sensitivity and acquired resistance in the context of therapeutic strategies that target oncogene addicted diseases.
HER2/neu癌基因是乳腺癌及其他癌症中重要的诊断、预后因素和治疗靶点。我们构建并鉴定了一种乳腺癌细胞系(Bam1a),该细胞系过表达活化的HER2/neu和ErbB-3,且具有与ErbB-2基因特征相符的基因表达谱。我们在体外和体内评估了表皮生长因子受体(EGFR)/HER2抑制剂吉非替尼对该乳腺肿瘤细胞系的作用。通过蛋白质印迹法表征了吉非替尼对EGFR、HER2和ErbB-3磷酸化的影响,并确定了其对生长、存活和应激途径下游信号传导的影响以及对增殖、细胞周期和凋亡的影响。吉非替尼处理以剂量依赖方式减少了ErbB-3>EGFR>HER2/neu以及转录信号转导子和激活子的磷酸化。通过丝裂原活化蛋白(MAP)/细胞外信号调节激酶激酶、p44/42 MAP激酶(MAPK)的下游促有丝分裂信号传导以及通过c-Jun-NH(2)-激酶(JNK)1和c-Jun的应激信号传导受损(1微摩尔/升,4 - 24小时),导致24小时内细胞生长停滞和细胞周期停滞,这是通过降低细胞周期蛋白D1、细胞周期蛋白B1和p(Ser795)Rb以及增加p27实现的。在0.5和1微摩尔/升时,增殖和集落形成分别受到抑制,且与基因表达谱改变相关。通过Akt的存活信号传导减弱、bim的诱导、连接蛋白43的丧失以及血管内皮生长因子-D的产生减少先于半胱天冬酶-3和聚(ADP)核糖聚合酶(PARP)的裂解和凋亡(>50% 2微摩尔/升,48小时)。口服吉非替尼能够阻止Bam1a肿瘤细胞从可触及病变中生长出来,缩小已形成的肿瘤,消除HER2和HER3磷酸化,并在体内降低MAPK和Akt信号传导。构建并鉴定了Bam1a细胞系的一个变体IR-5,其获得了在5微摩尔/升吉非替尼中生长的能力。IR-5在HER2/neu中存在一个新的点突变,该突变对应于ATP结合口袋中的L726I,与对吉非替尼敏感性的对数下降、与EGFR和HER3的异二聚化增加以及下调受损相关。IR-5的基因表达谱显示EMP-1、NOTCH-1、FLT-1、PDGFB和其他几个基因的表达增加,这些基因可能有助于耐药表型并通过MAPK和Akt维持信号传导。该模型将有助于理解在针对癌基因成瘾性疾病的治疗策略背景下,内在药物敏感性和获得性耐药之间的差异。
