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EGFR with TKI-sensitive mutations in exon 19 is highly expressed and frequently detected in Chinese patients with lung squamous carcinoma

机译:在中国肺鳞癌患者中外显子19中具有TKI敏感突变的EGFR高表达并经常被检测到

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摘要

Recently, tyrosine kinase inhibitors (TKIs) have been recommended as a first-line treatment for advanced non-small cell lung cancer (NSCLC), significantly improving the treatment outcomes of lung adenocarcinoma patients with the EGFR mutation. However, the application of TKIs for lung squamous cell carcinoma (SCC), the second largest pathological subtype of NSCLC, remains controversial because available data for the EGFR mutation profile and frequency in SCC patients are limited. In this study, 89 bronchoscopic–biopsy specimens from Chinese SCC male patients were assayed for EGFR exon 19 mutation, using improved polymerase chain reaction-denature gel gradient electrophoresis. EGFR exon 19 mutations were detected in 77 of 89 (86.5%) patients, and included six kinds of point mutations (11.6%) and two deletions (Del_747-751 [64.9%] and Del_746-751 [23.3%]). We found that the proportion of mutated EGFR varied from 0.98% to 100% in positive specimens and increased with the development of the disease. The difference of proportion between Stage IV patients and Stage II patients or Stage III patients was significant (P<0.001). These results provided valuable clues to explain the reason why patients harboring the same mutation responded distinctly to TKI treatment. Del_747-751 and Del_746-751 were the dominant mutations in the assayed SCC patients (76.4%), and both belong to the EGFR–TKI-sensitive mutation. Recently research demonstrated that Del_746-751 patients have better response to EGFR-TKI than Del_L747-751 patients. However, our study indicated that majority of SCC patients (55.5%) carried Del_ L747-751. We suggest that the unique clinic features of SCC should be further studied to reveal the mechanism of poorer treatment outcome of EGFR–TKI therapy, and that a better treatment plan and more specific, potent targeted drugs for lung SCC need to be developed.
机译:最近,酪氨酸激酶抑制剂(TKIs)已被推荐作为晚期非小细胞肺癌(NSCLC)的一线治疗,可显着改善具有EGFR突变的肺腺癌患者的治疗效果。然而,TKIs在NSCLC的第二大病理亚型肺鳞状细胞癌(SCC)中的应用仍存在争议,因为SCC患者中EGFR突变谱和频率的可用数据有限。在这项研究中,使用改良的聚合酶链反应-变性凝胶梯度电泳技术,对89位中国SCC男性患者的支气管镜活检标本进行了EGFR外显子19突变检测。在89例患者中检测到EGFR外显子19突变(86.5%),其中包括6种点突变(11.6%)和两个缺失(Del_747-751 [64.9%]和Del_746-751 [23.3%])。我们发现,在阳性样本中,EGFR突变的比例从0.98%到100%不等,并且随着疾病的发展而增加。 IV期患者与II期患者或III期患者之间的比例差异显着(P <0.001)。这些结果提供了有价值的线索,以解释具有相同突变的患者对TKI治疗产生明显反应的原因。 Del_747-751和Del_746-751是所分析的SCC患者的主要突变(76.4%),均属于EGFR-TKI敏感突变。最近的研究表明,与Del_L747-751患者相比,Del_746-751患者对EGFR-TKI的反应更好。但是,我们的研究表明,大多数SCC患者(55.5%)携带Del_ L747-751。我们建议应进一步研究SCC的独特临床特征,以揭示EGFR-TKI治疗不良治疗结果的机制,并需要制定更好的治疗计划和针对肺SCC的更具体,有效的靶向药物。

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