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首页> 外文期刊>Pathology Research and Practice >Characterization of common and rare mutations in EGFR and associated clinicopathological features in a large population of Chinese patients with lung cancer
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Characterization of common and rare mutations in EGFR and associated clinicopathological features in a large population of Chinese patients with lung cancer

机译:肺癌大量患者EGFR和相关临床病理特征中常见和罕见突变的特征

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摘要

Lung cancer with EGFR mutation is often associated pathological characteristics and good responses to EGFR tyrosine kinase inhibitors (TKIs). However, certain types of rare EGFR mutations have be linked to cases with poor response to EGFR TKIs. Therefore, extensive molecular screening and pathological characterization are essential for accurate diagnosis and selection of effective treatment plans. Although a large body of studies have established the rate of EGFR mutations as a whole entity, the rates of each individual types of mutations, especially those rare ones, have not been precisely determined in large patient populations with uniform genetic background. To address this issue, we assembled a large cohort of 456 Chinese patients with lung cancers to determine the rate of both common and rare forms of EGFR mutations and associated clinicopathological features in this retrospective study. We have found single or double EGFR mutations in 200 (43.9%) patients, including exon 19 deletions (E19del) (20%), exon 21 L858R (17.1%) and L861Q (1.5%) point mutations, exon 20 T790M (1.3%) and other mutations (1,3%), exon 18 mutations (1.3%), and double mutations (1.3%). EGFR mutation as well as its subtypes E19del, L858R, or double mutations were associated with female patients or never-smokers. In contrast, rare mutations, especially EGFR TKI resistant exon 20 mutations, were not statistically associated with any clinicopathological features, implicating that tumorigenesis driven by different EGFR mutations were mechanistically different. In summary, we have determined occurring rate of EGFR subtype mutations and demonstrated that different mutations showed different clinicopathological manifestations in lung cancer. (C) 2017 Elsevier GmbH. All rights reserved.
机译:具有EGFR突变的肺癌通常是相关的病理特征,对EGFR酪氨酸激酶抑制剂(TKI)的良好反应。然而,某些类型的稀有EGFR突变与对EGFR TKIS的响应不良的病例相关联。因此,广泛的分子筛查和病理表征对于准确的诊断和选择有效治疗计划至关重要。虽然大量的研究已经建立了作为整个实体的EGFR突变的速率,但是每个单独类型的突变的速率,尤其是那些罕见的突变,尚未精确地确定在具有均匀遗传背景的大型患者群体中。为了解决这个问题,我们组装了一个大量的456名中国肺癌患者患者,以确定这项回顾性研究中的常见和稀有形式的常见和罕见的临床病理学特征。我们在200名(43.9%)患者中发现了单一或双重EGFR突变,包括外显子19缺失(E19DEL)(20%),外显子21L858R(17.1%)和L861Q(1.5%)点突变,外显子20 T790M(1.3% )和其他突变(1,3%),外显子18突变(1.3%)和双突变(1.3%)。 EGFR突变以及其亚型E19DEL,L858R或双重突变与女性患者或非吸烟者有关。相反,罕见的突变,尤其是EGFR TKI抗性外显子20突变与任何临床病理特征没有统计学相关,这意味着由不同EGFR突变驱动的肿瘤发生在机械上不同。总之,我们已经确定了EGFR亚型突变的发生率,并证明了不同的突变在肺癌中显示出不同的临床病理表现。 (c)2017 Elsevier GmbH。版权所有。

著录项

  • 来源
    《Pathology Research and Practice》 |2017年第7期|共10页
  • 作者单位

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Sanford Burnham Prebys Med Discovery Inst 10901 N Torrey Pines Rd La Jolla CA 92037 USA;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

    Zhengzhou Univ Affiliated Tumor Hosp Henan Canc Hosp 127 Dongming Rd Zhengzhou 450008 Henan;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 病理学;
  • 关键词

    EGFR TKI; E19del; L858R; T790M; L861Q;

    机译:EGFR TKI;E19DEL;L858R;T790M;L861Q;

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