循环中c-met信使核糖核酸的过表达与非小细胞肺癌的淋巴结分期及早期复发显著相关。
Overexpression of circulating c-met messenger RNA is significantly correlated with nodal stage and early recurrence in non-small cell lung cancer.
作者信息
Cheng Tian-Lu, Chang Mei-Yin, Huang Sung-Yu, Sheu Chau-Chyun, Kao Eing-Long, Cheng Yu-Jen, Chong Inn-Wen
机构信息
MedicoGenomic Research Center, Kaohsiung Medical University, 100 Shih-Chuan First Rd, Kaohsiung, 807 Taiwan.
出版信息
Chest. 2005 Sep;128(3):1453-60. doi: 10.1378/chest.128.3.1453.
BACKGROUND
The c-met receptor and its ligand hepatocyte growth factor have been shown to be involved in tumor invasiveness and metastasis. Overexpression of c-met has been demonstrated in lung cancer tissues and cell lines, but the expression of c-met in peripheral blood (circulating c-met) has not been addressed. The molecular monitoring of circulating c-met could be helpful for selecting patients for adjuvant therapy.
OBJECTIVES
To investigate the expression of circulating c-met in non-small cell lung cancer (NSCLC) patients and to assess its prognostic implications.
METHODS
We quantified the levels of c-met messenger RNA (mRNA) in paired tumor and normal lung tissues and their peripheral bloods in 45 patients with NSCLC by real-time polymerase chain reaction (PCR). The expression status of c-met protein in tumor tissues was further evaluated by immunohistochemistry.
RESULTS
c-Met mRNA was significantly higher by 1.5 to 11 times in 34 of 45 tumor tissues (75.5%) than it was in their normal counterparts by real-time PCR. A comparison of this assay to immunohistochemistry suggested that real-time PCR was more sensitive than immunohistochemistry (27 of 45 tumor tissues, 60.0%) for the detection of c-met (p = 0.016). Of these patients with overexpression of c-met in tumors, 67.6% (23 of 34 patients) expressed higher amounts of circulating c-met by 1.4 to 8 times that of the normal control subjects. In addition, overexpression of circulating c-met was significantly correlated with nodal (N) stage (p = 0.011), but weakly correlated with tumor (T) stage (p = 0.056) and overall stages (p = 0.054) in patients with NSCLC. However, no correlations were found among circulating c-met and other factors such as age, gender, and pathologic types. Moreover, by univariate analysis, circulating c-met overexpression and pathologic stages (including T and N stages) were the most important factors correlated with early recurrence (p < 0.05). Only the circulating c-met remained as an independent predictor of early recurrence (hazard ratio, 3.94; 95% confidence interval, 1.17 to 13.33; p = 0.027) after Cox regression multivariate analysis.
CONCLUSIONS
Overexpression of circulating c-met is significantly correlated with the N stage and early recurrence. Moreover, early recurrence is frequently noted in patients with overexpression of circulating c-met, indicating that circulating c-met is an independent negative prognostic indicator in NSCLC.
背景
已证实c-met受体及其配体肝细胞生长因子与肿瘤侵袭和转移有关。在肺癌组织和细胞系中已证实c-met过表达,但外周血中c-met的表达(循环c-met)尚未得到研究。循环c-met的分子监测可能有助于选择辅助治疗的患者。
目的
研究非小细胞肺癌(NSCLC)患者循环c-met的表达,并评估其预后意义。
方法
我们通过实时聚合酶链反应(PCR)对45例NSCLC患者配对的肿瘤组织、正常肺组织及其外周血中的c-met信使核糖核酸(mRNA)水平进行了定量分析。通过免疫组织化学进一步评估肿瘤组织中c-met蛋白的表达状态。
结果
通过实时PCR检测,45例肿瘤组织中的34例(75.5%)c-Met mRNA水平显著高于其对应的正常组织,高出1.5至11倍。该检测方法与免疫组织化学的比较表明,实时PCR检测c-met的敏感性高于免疫组织化学(45例肿瘤组织中的27例,60.0%)(p = 0.016)。在这些肿瘤中c-met过表达的患者中,67.6%(34例患者中的23例)循环c-met表达量高出正常对照受试者1.4至8倍。此外,NSCLC患者中循环c-met过表达与淋巴结(N)分期显著相关(p = 0.011),但与肿瘤(T)分期(p = 0.056)和总分期(p = 0.054)的相关性较弱。然而,循环c-met与年龄、性别和病理类型等其他因素之间未发现相关性。此外,单因素分析显示,循环c-met过表达和病理分期(包括T和N分期)是与早期复发相关的最重要因素(p < 0.05)。在Cox回归多因素分析后,只有循环c-met仍然是早期复发的独立预测因子(风险比,3.94;95%置信区间,1.17至13.33;p = 0.027)。
结论
循环c-met过表达与N分期和早期复发显著相关。此外,循环c-met过表达的患者经常出现早期复发,这表明循环c-met是NSCLC中一个独立的负面预后指标。
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