颊黏膜细胞作为体内模型用于评估吉非替尼对晚期非小细胞肺癌患者的活性。
Buccal mucosa cells as in vivo model to evaluate gefitinib activity in patients with advanced non small cell lung cancer.
作者信息
Loprevite Maura, Tiseo Marcello, Chiaramondia Maurizio, Capelletti Marzia, Bozzetti Cecilia, Bortesi Beatrice, Naldi Nadia, Nizzoli Rita, Dadati Patrizia, Kunkl Annalisa, Zennaro Daniela, Lagrasta Costanza, Campanini Nicoletta, Spiritelli Elena, Camisa Roberta, Grossi Francesco, Rindi Guido, Franciosi Vittorio, Ardizzoni Andrea
机构信息
Medical Oncology A, National Institute for Cancer Research, S. Martino Hospital, Genoa, Italy.
出版信息
Clin Cancer Res. 2007 Nov 1;13(21):6518-26. doi: 10.1158/1078-0432.CCR-07-0805.
PURPOSE
To evaluate the role of pretreatment and posttreatment expression in buccal mucosa cells of signal transduction proteins activated by epidermal growth factor receptor, including phosphorylated epidermal growth factor receptor (p-EGFR), phosphorylated mitogen-activated protein kinase (p-MAPK), and phosphorylated AKT (p-AKT), in predicting gefitinib activity in advanced non-small cell lung cancer patients. Expression of the same proteins was also assessed on corresponding tissue samples for comparison. Moreover, EGFR gene mutations and copy number were analyzed.
EXPERIMENTAL DESIGN
Protein expression was evaluated by standard immunocytochemistry in buccal smears, obtained by scraping immediately before and after 2 weeks of gefitinib treatment, and in the available archival tumor specimens. EGFR gene mutations were evaluated by direct sequencing and gene copy number was determined by fluorescence in situ hybridization. Data were correlated with gefitinib toxicity and objective response.
RESULTS
Fifty-eight patients with pretreated advanced non-small cell lung cancer were enrolled and nine of these patients (15%) showed an objective response to gefitinib (including two complete responses). Toxicity (P = 0.025) and baseline p-AKT expression in buccal mucosa cells (P = 0.061) showed a potential predictive role. On the contrary, the probability of achieving an objective response was not affected by pretreatment expression of EGFR, p-EGFR, and p-MAPK, either in buccal mucosa or in tumor tissue. Responders showed a nonstatistically significant trend toward a more pronounced reduction in the expression of p-EGFR, p-MAPK, and p-AKT after gefitinib treatment. Among responders, five of six (83%) tumors showed EGFR gene mutation, whereas none of the tumors from patients with stable or progressive disease did (P < 0.001).
CONCLUSIONS
Epithelial cells obtained from buccal mucosa may be used to assess the pharmacodynamic effect of EGFR-targeted agents, and pretreatment p-AKT expression may be a possible predictive biomarker of in vivo gefitinib activity.
目的
评估表皮生长因子受体激活的信号转导蛋白(包括磷酸化表皮生长因子受体(p-EGFR)、磷酸化丝裂原活化蛋白激酶(p-MAPK)和磷酸化AKT(p-AKT))在治疗前和治疗后的颊黏膜细胞中的表达,在预测晚期非小细胞肺癌患者吉非替尼活性中的作用。还对相应组织样本中相同蛋白的表达进行评估以作比较。此外,分析了表皮生长因子受体(EGFR)基因突变和拷贝数。
实验设计
通过标准免疫细胞化学评估蛋白表达,检测样本包括吉非替尼治疗前和治疗2周后立即刮取的颊黏膜涂片,以及可用的存档肿瘤标本。通过直接测序评估EGFR基因突变,通过荧光原位杂交确定基因拷贝数。数据与吉非替尼毒性和客观缓解情况相关联。
结果
纳入58例接受过治疗的晚期非小细胞肺癌患者,其中9例患者(15%)对吉非替尼显示出客观缓解(包括2例完全缓解)。毒性(P = 0.025)和颊黏膜细胞中的基线p-AKT表达(P = 0.061)显示出潜在的预测作用。相反,无论在颊黏膜还是肿瘤组织中,治疗前EGFR、p-EGFR和p-MAPK的表达均不影响获得客观缓解的概率。缓解者在吉非替尼治疗后p-EGFR、p-MAPK和p-AKT的表达有更明显降低的趋势,但无统计学意义。在缓解者中,六分之五(83%)的肿瘤显示EGFR基因突变,而疾病稳定或进展患者的肿瘤均未显示该突变(P < 0.001)。
结论
从颊黏膜获取的上皮细胞可用于评估表皮生长因子受体靶向药物的药效学效应,治疗前p-AKT表达可能是体内吉非替尼活性的一种可能的预测生物标志物。
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