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彭明政 彭菲 李钊 周建华 林强.肺磨玻璃结节中ki-67 的表达及与P53, EGFR, CEA相关性研究[J].现代生物医学进展英文版,2015,15(32):6206-6211.
肺磨玻璃结节中ki-67 的表达及与P53, EGFR, CEA相关性研究
The Expression of ki-67 in Ground-glass Opacity (GGO) and its Relationwith P53, EGFR, CEA
  
DOI:
中文关键词: 肺磨玻璃结节  GGO  ki-67  p53  ROC
英文关键词: Ground-glass opacity  ki-67  Correlation  p53  ROC
基金项目:国家自然科学基金项目(81372521)
Author NameAffiliation
彭明政 彭菲 李钊 周建华 林强 上海交通大学附属第一人民医院胸外科湖南师范大学医学院附属湖南省人民医院 
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中文摘要:
      目的:为探究不同病理类型的肺磨玻璃结节(ground-glass opacity, GGO)中ki-67 的表达情况及其与肺癌相关标志物p53、 p63、EGFR 等表达的相关性。方法:收集从2012 年10 月至2014 年10 月我院胸外科收治的254 例GGO病人的临床病史、影像、 病理及血常规等资料予以回顾性分析。结果:Ki-67表达量从良性组(n=66),不典型腺瘤样增生(atypical adenomatous hyperplasia, AAH, n=27),到原位癌(adenocarcinoma in situ, AIS, n=11),微浸润腺癌(minimally invasive adenocarcinoma, MIA, n=108),最后到 浸润性腺癌(invasive adenocarcinoma, IAC, n=42)即随着早期肺癌的演进过程不断增高。Ki-67 与各标志物的相关系数为0.386 (p53, P<0.001)、0.227(EGFR, P=0.024)、0.441(CEA, P<0.001)。通过ROC 曲线分析得到ki-67 来判别良恶性GGO 的曲线下面积 和最佳阈值,也得到了早期肺癌演进过程中ki-67 阈值变化。恶性GGO 组全血细胞中平均单核细胞含量低于良性组GGO,且差 异有统计学意义。结论:ki-67 表达量在不同病理类别的GGO中有显著性差异,且在肺癌演进过程中依次增高,可作为鉴别早期 肺癌不同病理类型的参考依据和预后因子;ki-67 与P53、EGFR 及CEA的表达具有一定的相关性。
英文摘要:
      Objective:To explore the expression of ki-67 in the GGO of different pathology and try to find whether the correlation of ki-67 with P53, EGFR and CEA.Methods:The clinical history, CT information, white blood cell count and pathology material of 254 cases with GGO during 2012 and 2014 were collected and analyzed retrospectively.Results:The expression level of ki-67 was gradually increased fromBenign group (n=66), AAH (n=27), AIS (n=11), MIA (n=108), to IAC (n=42) , which is exactly the evolution progression of early lung adenocarcinoma; The correlation coefficient were 0.386 (p53, P<0.001), 0.227(EGFR, P=0.024) and 0.441 (CEA, P<0.001) respectively; By ROC curve analysis, we got the AUC and optimal cut-off points of ki-67 with regarding to differentiation of GGO and the variation of thresholds along the progression of early lung adenocarcinoma; The number and the percentage of blood monocyte of the patients with malignant GGO were lower than these of benign group.Conclusion:There are significant differences among GGOs of different pathologic categories with respect to the expression of ki-67 that gradually increased in the early lung adenocarcinoma progression. To some extent, a positive correlation of ki-67 with P53, EGFR and CEA exists.
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