Ozlem Sherif, Said A Khelwatty, Izhar Bagwan, Alan M Seddon, Angus Dalgleish, Satvinder Mudan, Helmout Modjtahedi
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At a cut off value of >5% of tumour cells stained for these biomarkers, 35% [wild‑type (wt)EGFR], 58% (HER‑2), 0% (HER‑3), 19% (HER‑4), 26% (EGFRvIII), 40% (CD44) and 33% (EpCAM) of patients were positive. In 23, 14 and 9% of the patients, wtEGFR expression was accompanied by co‑expression with HER‑2, EGFRvIII and HER‑2/EGFRvIII, respectively. EGFRvIII expression, membranous expression of CD44 and co‑expression of wtEGFR/EGFRvIII were associated with poor overall survival (OS). By contrast, cytoplasmic CD44 expression was associated with a longer OS time. The present study also investigated the effect of several agents targeting one or more members of the HER family, other growth factor receptors and cell signalling proteins on the proliferation of HCC cell lines. Among agents targeting one or more members of the HER family, the pan‑HER family blocker afatinib was the most effective, inhibiting the proliferation of three out of seven human liver cancer cell lines (LCCLs), while the CDK inhibitor dinacicilib was the most effective agent, inhibiting the proliferation of all human LCCLs tested. Taken together, the present results suggested that EGFRvIII expression and its co‑expression with wtEGFR or CD44 was of prognostic significance. 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At present, several HER inhibitors have been approved for the treatment of patients with a range of cancers but not for the treatment of patients with hepatocellular carcinoma (HCC). The present study investigated the co‑expression and prognostic significance of HER family members, type‑III deletion mutant EGFR (EGFRvIII), and the putative CSC biomarkers CD44 and epithelial cell adhesion molecule (EpCAM) in 43 patients with HCC. The relative expression of these biomarkers was determined using immunohistochemistry. At a cut off value of >5% of tumour cells stained for these biomarkers, 35% [wild‑type (wt)EGFR], 58% (HER‑2), 0% (HER‑3), 19% (HER‑4), 26% (EGFRvIII), 40% (CD44) and 33% (EpCAM) of patients were positive. In 23, 14 and 9% of the patients, wtEGFR expression was accompanied by co‑expression with HER‑2, EGFRvIII and HER‑2/EGFRvIII, respectively. 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引用次数: 0
摘要
HER家族成员和癌症干细胞(CSC)的异常表达与肿瘤进展和抗药性有关。目前,几种HER抑制剂已被批准用于治疗多种癌症患者,但尚未用于治疗肝细胞癌(HCC)患者。本研究调查了43例HCC患者中HER家族成员、III型表皮生长因子受体缺失突变体(EGFRvIII)以及假定的CSC生物标志物CD44和上皮细胞粘附分子(EpCAM)的共同表达和预后意义。这些生物标记物的相对表达采用免疫组化法测定。在肿瘤细胞对这些生物标记物染色>5%的临界值下,35%的患者[野生型(wt)表皮生长因子受体]、58%的患者(HER-2)、0%的患者(HER-3)、19%的患者(HER-4)、26%的患者(表皮生长因子受体vIII)、40%的患者(CD44)和33%的患者(EpCAM)呈阳性。在 23、14 和 9% 的患者中,wtEGFR 的表达分别与 HER-2、EGFRvIII 和 HER-2/EGFRvIII 同时表达。表皮生长因子受体vIII的表达、CD44的膜表达和wtEGFR/EGFRvIII的共表达与总生存率(OS)低下有关。相比之下,细胞质 CD44 表达与较长的 OS 时间相关。本研究还调查了几种靶向 HER 家族一个或多个成员、其他生长因子受体和细胞信号转导蛋白的药物对 HCC 细胞株增殖的影响。在靶向HER家族一个或多个成员的药物中,泛HER家族阻断剂阿法替尼最有效,抑制了7个人类肝癌细胞系(LCCLs)中3个细胞系的增殖,而CDK抑制剂地那西利是最有效的药物,抑制了所有受试人类LCCLs的增殖。综上所述,本研究结果表明,表皮生长因子受体阻断因子 vIII 的表达及其与 wtEGFR 或 CD44 的共表达对预后具有重要意义。这些结果也支持进一步研究针对 EGFRvIII 和 HER 家族其他成员的药物对 HCC 患者的治疗潜力。
Expression of EGFRvIII and its co‑expression with wild‑type EGFR, or putative cancer stem cell biomarkers CD44 or EpCAM are associated with poorer prognosis in patients with hepatocellular carcinoma.
The aberrant expression of HER family members and cancer stem cells (CSCs) have been associated with tumour progression and resistance to therapy. At present, several HER inhibitors have been approved for the treatment of patients with a range of cancers but not for the treatment of patients with hepatocellular carcinoma (HCC). The present study investigated the co‑expression and prognostic significance of HER family members, type‑III deletion mutant EGFR (EGFRvIII), and the putative CSC biomarkers CD44 and epithelial cell adhesion molecule (EpCAM) in 43 patients with HCC. The relative expression of these biomarkers was determined using immunohistochemistry. At a cut off value of >5% of tumour cells stained for these biomarkers, 35% [wild‑type (wt)EGFR], 58% (HER‑2), 0% (HER‑3), 19% (HER‑4), 26% (EGFRvIII), 40% (CD44) and 33% (EpCAM) of patients were positive. In 23, 14 and 9% of the patients, wtEGFR expression was accompanied by co‑expression with HER‑2, EGFRvIII and HER‑2/EGFRvIII, respectively. EGFRvIII expression, membranous expression of CD44 and co‑expression of wtEGFR/EGFRvIII were associated with poor overall survival (OS). By contrast, cytoplasmic CD44 expression was associated with a longer OS time. The present study also investigated the effect of several agents targeting one or more members of the HER family, other growth factor receptors and cell signalling proteins on the proliferation of HCC cell lines. Among agents targeting one or more members of the HER family, the pan‑HER family blocker afatinib was the most effective, inhibiting the proliferation of three out of seven human liver cancer cell lines (LCCLs), while the CDK inhibitor dinacicilib was the most effective agent, inhibiting the proliferation of all human LCCLs tested. Taken together, the present results suggested that EGFRvIII expression and its co‑expression with wtEGFR or CD44 was of prognostic significance. These results also support further investigations of the therapeutic potential of drugs targeting EGFRvIII and other members of the HER family in patients with HCC.
期刊介绍:
Oncology Reports is a monthly, peer-reviewed journal devoted to the publication of high quality original studies and reviews concerning a broad and comprehensive view of fundamental and applied research in oncology, focusing on carcinogenesis, metastasis and epidemiology.