Cyclooxygenase-2 and epithelial growth factor receptor up-regulation during progression of Barrett's esophagus to adenocarcinoma

AIM： To investigate the expression of cyclooxygenase-2 （COX-2） and epithelial growth factor receptor （EGFR） throughout the progression of Barrett＇s esophagus （BE）. METHODS： COX-2 and EGFR protein expressions were detected by using immunohistochemical method. A detailed cytomorphological changes were determined. Areas of COX-2 and EGFR expression were quantified by using computer Imaging System. RESULTS： The expressions of both COX-2 and EGFR increased along with the progression from BE to esophagus adenocarcinoma （EAC）. A positive correlation was found between COX-2 expression and EGFR expression. CONCLUSION： COX-2 and EGFR may be cooperative in the stepwise progression from BE to EAC, thereby leading to carcinogenesis.

Treatment of gastrointestinal neuroendocrine tumors with inhibitors of growth factor receptors and their signaling pathways: Recent advances and future perspectives

The limited efficacy of conventional cytotoxic treatment regimes for advanced gastrointestinal neuroendocrine cancers emphasizes the need for novel and more effective medical treatment options. Recent findings on the specific biological features of this family of neoplasms has led to the development of new targeted therapies, which take into account the high vascularization and abundant expression of specific growth factors and cognate tyrosine kinase receptors. This review will briefly summarize the status and future perspectives of antiangiogenic, mTOR- or growth factor receptor-based pharmacological approaches for the innovative treatment of gastrointestinal neuroendocrine tumors. In view of the multitude of novel targeted approaches, the rationale for innovative combination therapies, i.e. combining growth factor (receptor)-targeting agents with chemo- or biotherapeutics or with other novel anticancer drugs such as HDAC or proteasome inhibitors will be taken into account.

Inhibition of epidermal growth factor receptor signaling protects human malignant glioma cells from hypoxia - induced cell death

Epidermal growth factor receptor(EGFR)signaling has become an importanttarget for drug development becauseEGFR signaling enhances tumor cell proliferation,migration,and invasion and inhibits apoptosis.However,theresults of clinical trials using EGFR inhibitors in patients with solid tumors have been disappointing.Here,wereport a protective effect of the EGFR inhibitors AG1478 and PD153035 against cell death induced by acute hy-poxia,which contrasts with their proapoptotic effects under normoxia.Under hypoxic conditions,both agents re-

Epidermal growth factor receptor-targeted immune magnetic liposomes capture circulating colorectal tumor cells efficiently

AIM To compare the capacity of newly developed epidermal growth factor receptor(EGFR)-targeted immune magnetic liposomes(EILs) vs epithelial cell adhesion molecule(Ep CAM) immunomagnetic beads to capture colorectal circulating tumor cells(CTCs).METHODS EILs were prepared using a two-step method, and the magnetic and surface characteristics were confirmed. The efficiency of capturing colorectal CTCs as well as the specificity were compared between EILs and Ep CAM magnetic beads. RESULTS The obtained EILs had a lipid nanoparticle structure similar to cell membrane. Improved binding with cancer cells was seen in EILs compared with the method of coupling nano/microspheres with antibody. The binding increased as the contact time extended. Compared with Ep CAM immunomagnetic beads, EILs captured more CTCs in peripheral blood from colorectal cancer patients. The captured cells showed consistency with clinical diagnosis and pathology. Mutation analysis showed same results between captured CTCs and cancer tissues. CONCLUSION EGFR antibody-coated magnetic liposomes show high efficiency and specificity in capturing colorectal CTCs.

The effect of low-dose total body irradiation on tumor-inhibition and signal transduction in tumor tissues of mice bearing S180 sarcoma

Objective： By studying the influence of low-dose total body irradiation to proliferating cell nuclear antigens （PCNA）, epidermal growth factor receptor （EGFR）, erythropoietin （EPO） and vascular endothelial growth factor receptor （VEGFR） of tumor tissues in mice bearing S180 sarcoma, to further explore the mechanism of low doses radiation. Methods：S180 sarcoma cells were implanted subcutaneously into 58 male Kunming mice. Randomly these mice were divided into sham-irradiation （S） group and low-dose radiation （LDR） group. 12 days after implantation, the mice in LDR group were once delivered 75 mGy total-body ^60Co y-ray irradiation, while the mice in S group were left without irradiation. Then the mice in LDR group were executed at 6 h （LDR-6h group）, 12 h （LDR-12 h group）, 24 h （LDR-24 h group）, 48 h （LDR-48 h group） and 72 h （LDR-72h group） after irradiation. Tumor tissues were weighed and histological observed. Immunohistochemical staining was used to detect the expression of PCNA, VEGF, EPO and VEGFR of tumor tissues. Results： Though there was no significant difference between LDR group and S group in tumor weight, after irradiation the expression of PCNA and EPO of tumor tissues in LDR group decreased with time. LDR-24h, LDR-48h and LDR-72h groups were all statistically significantly different from S group. The expression of EGFR and VEGFR also decreased, and LDR-24h group was the lowest （P 〈 0.05）. Conclusion： Seventy-two h after low-dose total body irradiation, there was no significant change in tumor size of mice bearing S180 sarcoma. Low-dose total body radiation decreased the expression of PCNA inhibiting tumor growth; reduced the expression of EGFR in tumor tissue impacting the signal transduction of tumor cells. The study also indicated that low-dose total body irradiation, within a certain period of time, can decrease the expression of hypoxia factor EPO and VEGFR, which may improve the situation of tumor hypoxia and radiosensitivity of tumor itself.

EGFR inhibitors sensitize non-small cell lung cancer cells to TRAIL-induced apoptosis

Apoptosis induced by tumor necrosis factor-related apoptosis-inducing ligand(TRAIL) can be regulated by the epidermal growth factor(EGF) signaling pathway.In this study,recombinant adenoviral vectors that encode TRAIL gene from the hTERT/RGD promoter(AdTRAIL) was combined with drugs including gefitinib,elotinib,and cetuximab that inhibit EGFR and the EGF signaling pathway in non-small cell lung cancer(NSCLC) cell lines to investigate their antitumor activity.In vitro,compared to single reagent,AdTRAIL combined with EGFR inhibitors reduced proliferation and enhanced apoptosis in H460,A549,and SW1573 cell lines.Western blot results suggested that these effects were relative to up-regulation of pro-apoptosis protein BAX and down-regulation of p-AKT.In vivo,AdTRAIL combined with cetuximab resulted in a significant growth reduction in H460 xenografts without damage to the main organs of nude mice.Histological examination and TUNEL analyses of xenografts showed that cetuximab enhanced cell apoptosis induced by AdTRAIL.These results indicate that EGFR inhibitors enhanced AdTRAIL anti-tumor activity in NSCLC cell lines and that inhibiting the AKT pathway played an important role in this enhancement.

EGFR Mutation and FHIT Methylation: Inverse Relationship in Patients with Lung Adenocarcinoma and Tuberculosis

Objective:To investigate the genetic correlations between epithelial growth factor receptor(EGFR)mutation and FHIT methylation in patients diagnosed with lung adenocarcinoma(AC)and pulmonary tuberculosis(TB).Methods:The presence of EGFR mutations and the methylation status of the FHIT gene in patients presenting with AC and TB were analyzed.The correlation between TB status and the observed genetic and epigenetic variations was also examined.Results:Among the 90 patients included in the study,38 exhibited EGFR mutations(14 among those with TB and 24 among those without TB),while 29 exhibited FHIT myelination(19 among those with TB and 10 among those without TB).Furthermore,the protein expression levels of EGFR and FHIT were significantly higher in patients diagnosed solely with AC compared to those presenting with both AC and TB.A robust inverse correlation was identified between TB status and the frequency of EGFR mutation(P<0.001).Moreover,significant associations were observed between TB status and FHIT methylation(P<0.01).Conclusion:The findings suggest a correlation between TB and the prevalence of EGFR mutation and FHIT methylation in the pathogenesis of AC.

EGFR和E-cadherin在食管癌组织中的表达及两者的相关性

背景与目的表皮生长因子受体(epithel ialgrowth factor receptor,EGFR)表达增高及表皮钙粘蛋白(E-cadherin)表达降低与肿瘤的发生、发展、侵袭、转移密切相关,但二者在食管癌病变中的表达报道较少,尤其二者在食管癌中相互关系的研究目前尚未见报道。本研究旨在探讨食管癌组织中EGFR和E-cadherin的表达水平,并分析二者的相互关系。方法采用免疫组织化学方法检测50例食管鳞癌、8例食管腺癌标本中EGFR和E-cadherin的表达水平。结果食管鳞癌中,EGFR和E-cadherin的阳性率分别为72.0%(36/50)、22.0%(11/50),在食管腺癌中分别为75.0%(6/8)、25.0%(2/8);EGFR和E-cadherin的表达强度之间呈明显负相关(r=-0.341,P=0.008)。结论食管癌组织中EGFR表达增高,E-cadherin表达降低;E-cadherin的表达水平降低可能与EGFR的高表达有关。

Dukes' A、B期结直肠癌c-erbB-2,EGFR和TGF-α表达与复发转移的关系

背景与目的:尽管病理分期是结直肠癌患者主要的预后指标,但目前的分期系统不足以预测Dukes' A、B期患者术后复发风险及指导辅助治疗。分子预后标志物有可能补充分期的不足,且能为基于肿瘤个体生物学特征的治疗决策提供依据。本研究旨在探讨Dukes' A、B期结直肠癌中c-erbB-2、表皮生长因子受体(epithelial growth factor receptor,EGFR)、转化生长因子α(transforming growth factor-α,TGF-α)表达与术后复发转移的关系。方法:收集中山大学肿瘤防治中心1989年～1999年间88例行根治性手术的结直肠腺癌病例,Dukes' A期26例,Dukes' B期62例,复发转移组和非复发转移组各44例。至少随访5年或随访至复发。应用免疫组化方法检测原发瘤组织中c-erbB-2、EGFR、TGF-α蛋白表达。结果:复发组c-erbB-2、EGFR、TGF-α过表达率分别为43.2%(19/44)、63.6%(28/44)、65.9%(29/44),非复发组阳性率分别为25.0%(11/44)、27.3%(12/44)、43.2%(19/44)。χ2检验提示复发组EGFR、TGF-α过表达率明显高于非复发组,但两组c-erbB-2过表达率无差异。复发组EGFR和TGF-α共同过表达率36.4%(16/44)显著高于非复发组11.4%(5/44)(χ2=7.568,P=0.006)。多因素分析显示EGFR表达与术后复发转移有关。结论:EGFR表达可能与Dukes’A、B期结直肠癌术后复发转移有关。

表现为磨玻璃样病变的肺腺癌临床特点与EGFR及K-RAS基因突变的关系

目的探讨表现为磨玻璃样病变(GGO)的肺腺癌的临床特点与EGFR及K-RAS基因突变关系。方法连续选择37例经胸腔镜手术及病理证实为肺腺癌的肺GGO病例,分析其临床特点,检测EGFR与K-RAS基因突变情况,及与各临床因素之间的关系。结果 34例行肺叶切除术,3例行肺楔形切除术,术后病理结果显示:16例为原位腺癌,13例为微浸润腺癌,8例为浸润性腺癌。EGFR基因突变22例,K-RAS基因突变1例;在单纯型GGO及混合型GGO病例中,EGFR与K-RAS基因突变均无明显差异;在女性、不吸烟病例中EGFR基因突变相较男性及吸烟病例差异具有统计学意义(P<0.05)。结论 EGFR基因在表现为GGO的肺腺癌病例中表现出较高的突变率,为肺GGO病例临床治疗提供了重要参考。

EGFR/STAT信号通路相关蛋白在特发性肺纤维化中的表达及临床意义

目的通过检测特发性肺纤维化(IPF)患者肺组织中表皮生长因子受体(EGFR)、细胞外调节蛋白酶(ERK1/2)和信号传导转录激活因子(STAT1)的表达,探讨与IPF临床特征及预后的关系。方法选择15例IPF患者及10例正常肺组织标本,经石蜡包埋切片后,行免疫组化检测,并与肺功能等检测指标结果进行分析。结果 IPF肺组织中EGFR和STAT1呈阳性表达分别为11/15例、10/15例,且两者表达与IPF患者肺总量、弥散功能及PaO2水平呈显著正相关(P<0.05),与IPF病理特征和高分辨率胸部CT影像特征之间无显著相关性;而在10例对照组肺组织中EGFR和STAT1均无明显阳性表达;IPF肺组织中RAS/MAPK信号转导分子ERK1/2表达水平较对照组肺组织无明显增强(P>0.05)。结论 EGFR/STAT1信号通路活化与IPF的发生、发展密切相关,可作为诊断和评估IPF进展的有价值的指标。

非小细胞肺癌原发灶与脑转移灶EGFR基因突变状况的一致性研究

目的探讨非小细胞肺癌(NSCLC)原发灶与脑转移灶的表皮生长因子受体(EGFR)基因突变状况,分析两者之间是否存在一致性。方法收集2003年1月至2011年12月31例NSCLC脑转移患者的肺原发灶和脑转移灶石蜡包埋组织标本,应用DNA直接测序法进行EGFR突变分析,如发现两者突变不一致则进一步采用增殖阻碍突变系统(ARMS)验证。结果 31例NSCLC肺原发灶中,8例存在19外显子E746-A750缺失突变、4例为21外显子L858R点突变;在31例脑转移灶样本中,8例为19外显子E746-A750缺失突变,3例存在21外显子L858R点突变,EGFR突变类型在脑转移灶和肺原发灶的分布差异无统计学意义(P=0.793)。共有16.1%(5/31)的肺原发灶和脑转移灶EGFR突变状况不一致,其中男性4例,女性1例;3例腺癌(2例脑转移灶19外显子缺失突变而肺原发灶阴性突变,1例肺原发灶21外显子点突变而脑转移灶阴性突变),1例鳞癌和1例非典型类癌(均为脑转移灶阴性突变而肺原发灶19外显子缺失突变)。结论 NSCLC原发病灶及脑转移灶EGFR基因突变存在不一致性。

非小细胞肺癌患者外周血游离DNA中检测EGFR基因突变

目的检测非小细胞肺癌患者外周血游离DNA中表皮生长因子受体(EGFR)基因19和21外显子的突变情况,并与相应的肿瘤组织检测结果进行比较,探讨非小细胞肺癌患者应用外周血游离DNA检测EGFR突变的临床意义。方法应用实时荧光聚合酶链反应(PCR)技术检测32例非小细胞肺癌患者术后肿瘤组织和术前外周血游离DNA中EGFR基因19和21外显子的突变,所有扩增标本均经基因测序法验证。结果 32份外周血标本中,共检测到13份EGFR基因突变,突变率达40.6%,肿瘤组织中有16份EGFR基因突变,突变率达50.0%,外周血和肿瘤组织EGFR基因同时突变的有13份,两者突变一致性达到81.2%,两者间差异无统计学意义(P>0.05)。结论外周血游离DNA代替肿瘤组织进行EGFR基因突变检测具有可行性,为无法取得肿瘤组织的非小细胞肺癌患者提供一种更快捷、简便的EGFR基因突变检测方法,其检测结果可为临床选择靶向药物治疗提供依据。

三阴性乳腺癌细胞中上皮间质转化与EGFR单抗治疗效果的相关性

目的研究三阴性乳腺癌(triple negative breast cancer,TNBC)细胞株的上皮间质转化(epithelial-mesenchymal transition,EMT)水平与西妥昔单抗药敏性的相关性。方法 (1)运用免疫印记法比较TNBC细胞株中EGFR、波形蛋白(vimentin)以及E钙黏蛋白(E-cadherin)的表达水平。(2)通过CCK8试剂比较不同细胞株对西妥昔单抗的敏感度。(3)采用Ⅰ型组蛋白去乙酰化酶抑制剂恩替诺特(ENT)逆转MDA-MB231的EMT。(4)观察ENT联合西妥昔单抗对MDA-MB231细胞活性的抑制作用。结果 (1)MDA-MB468细胞中E-cadherin的表达水平明显高于MDA-MB436及MDAMB231细胞;vimentin的表达水平明显低于MDA-MB436及MDA-MB231。(2)MDA-MB468对西妥昔单抗的敏感度明显高于MDA-MB231及MDA-MB436。(3)MDA-MB231的EMT能被Ⅰ型组蛋白去乙酰化酶抑制剂ENT逆转。(4)ENT单药显著抑制MDA-MB231细胞的活性,ENT联合西妥昔单抗较ENT单药对细胞生长的抑制作用更加显著。结论 TNBC细胞中,EMT与EGFR单克隆抗体西妥昔单抗的疗效可能相关。联合Ⅰ型组蛋白去乙酰化酶抑制剂ENT以及西妥昔单抗治疗可能是治疗TNBC的新方法。

细胞膜色谱在线HPLC-IT-TOF MS联用系统筛选分析射干中次野鸢尾黄素的抗EGFR活性作用

中药射干具有多种药理作用并得到广泛研究,但对其抗肿瘤活性组分的研究较少。本研究建立了一种用于筛选射干中抗肿瘤活性组分的方法。利用高表达表皮生长因子受体(EGFR)细胞制备细胞膜色谱柱,并通过十通切换阀与高效液相色谱-离子阱-飞行时间质谱(HPLC-IT-TOF MS)构建成二维在线联用系统。利用吉非替尼验证该系统的适用性,分子模拟对接实验研究活性组分与受体的相互作用方式,并利用MTT实验研究所筛选组分对EGFR细胞的体外抑制作用。结果表明,利用该系统可从射干总提取物中筛选出能够作用于EGFR的活性成分,并鉴定为次野鸢尾黄素;次野鸢尾黄素与EGFR的相互作用方式与阳性药吉非替尼相似;在浓度为0.4~50μmol/L范围内,吉非替尼、次野鸢尾黄素对高表达EGFR细胞的体外抑制作用具有剂量依赖性。EGFR细胞膜色谱在线HPLC-IT-TOF MS法有望成为从中草药中发现潜在抗肿瘤候选药物的有效方法。

晚期非小细胞肺癌EGFR基因突变及其与患者临床特征的相关性

目的探索晚期非小细胞肺癌(NSCLC)患者中EGFR基因状态与患者临床特征的内在关系。方法回顾性分析西安市中心医院肿瘤科2015年1月至2018年12月收治的72例初诊晚期NSCLC患者的临床资料,统计其EGFR基因突变、性别、吸烟、病理类型、淋巴结转移、首发远处转移灶以及癌胚抗原(CEA)、神经元特异性烯醇化酶(NSE)、细胞角蛋白19片段(Cy211)等指标,分析EGFR基因突变情况与上述各项指标的相关性。结果 72例初诊晚期NSCLC患者的EGFR基因总体突变率为44.44%。不吸烟患者的EGFR基因突变率为60.00%(21/35),高于吸烟患者的29.73%(11/37),差异有统计学意义(P<0.05);不同病理类型肺癌中的EGFR基因突变率也不同,腺癌中EGFR基因突变率最高,腺鳞癌次之,鳞癌最低,差异有统计学意义(P<0.05);有淋巴结转移的NSCLC患者的EGFR基因突变率为70.83%,明显高于无淋巴结转移的31.25%,差异有统计学意义(P<0.05);EGFR基因突变的NSCLC患者脑部转移发生率高于其他部位,EGFR基因突变与脑转移之间呈中度正相关(r=0.491,P<0.05),而与骨转移呈中度负相关(r=-0.47,P<0.05);CEA及Cy211在EGFR基因突变患者中表达均值分别为(6.75±3.44) ng/mL、(9.82±7.34)μg/L,而在EGFR野生型患者中的CEA及Cy211的表达均值分别为(14.73±14.29) ng/mL、(28.51±24.54)μg/L,CEA及Cy211在EGFR野生型患者中的表达水平更高,两组间比较差异均有统计学意义(P<0.05)。结论晚期NSCLC患者中EGFR基因的突变率整体较高,EGFR基因突变与患者的临床特征相关,腺癌、非吸烟人群、淋巴结转移等临床特征的患者更易携带EGFR基因的突变;EGFR基因突变与脑转移成正相关,但与骨转移成负相关。此外,低表达CEA及Cy211可能与EGFR突变有相关性,可作为预测EGFR基因是否突变的参考指标。

EGFR和SBEM联合检测在乳腺癌外周血微转移中的意义

目的:探讨乳腺癌患者外周血表皮生长因子受体(EGFR)及乳腺上皮粘蛋白(SBEM)的表达及临床意义。方法:采用酶联免疫吸附试验(ELISA法)定量检测58例乳腺癌患者及30例乳腺纤维腺瘤患者术前血清中EGFR和SBEM的含量。结果:乳腺癌组术前血清EGFR和SBEM含量均高于纤维腺瘤对照组(P<0.01)。有淋巴结转移的乳腺癌患者血清中EGFR和SBEM含量明显高于无淋巴结转移者,Ⅲ+Ⅳ期患者血清中EGFR和SBEM含量亦显著高于Ⅰ+Ⅱ期,差异均有统计学意义(P<0.05)。乳腺癌患者术前血清中EGFR和SBEM含量无相关性(r=-0.45,P=0.74)。结论:EGFR及SBEM特异性表达于乳腺癌外周血,有可能作为检测乳腺癌外周血微转移的标志物,并有可能在乳腺癌微转移诊断和预后判断中具有重要意义。

浸润性乳腺癌PTEN、p53、EGFR与ER、PR及HER-2表达的关系

目的研究乳腺癌中雌激素受体(ER)、孕激素受体(PR)、表皮生长因子受体2(HER-2)与丢失性磷酸酶-张力蛋白基因(PTEN)、蛋白p53、表皮生长因子受体(EGFR)的关系。方法采用免疫组织化学S-P法检测ER、PR、HER-2、PTEN、p53和EGFR在68例乳腺浸润性癌和10例乳腺纤维腺瘤组织标本中的表达。结果 ER、PR、HER-2、PTEN、p53和EGFR的表达分别是44.1%、47.1%、54.4%、45.6%、51.5%、58.8%,PTEN蛋白表达与ER呈正相关;p53蛋白表达与ER、PR表达呈负相关;EGFR的表达与ER呈负相关、与HER-2呈正相关。结论联合检测ER、PR、HER-2、PTEN、p53、EGFR对临床上乳腺癌患者判断预后和靶向治疗有重要临床意义。

Hck基因通过EGFR通路对肺腺癌细胞增殖和侵袭能力的影响

目的探讨造血细胞激酶(Hck)基因对肺腺癌A-549细胞增殖和侵袭的影响及机制。方法利用干扰和过表达Hck质粒转染A-549细胞,用MTT法检测细胞增殖能力,Transwell小室检测细胞侵袭能力,细胞划痕试验检测细胞迁移能力,RT-PCR法检测Hck和上皮生长因子受体(EGFR)mRNA表达水平,Western blot法检测Hck和EGFR蛋白表达水平。RT-PCR法检测18例临床肺腺癌组织和癌旁组织中Hck和EGFR mRNA表达水平,Pearson法分析Hck mRNA和EGFR mRNA的相关性。结果过表达Hck后A-549细胞增殖能力、侵袭能力和迁移能力均升高(P <0.05),EGFR mRNA和蛋白表达水平也有所升高(P <0.05);干扰Hck表达后A-549细胞增殖能力、侵袭能力和迁移能力均下降(P <0.05),EGFR mRNA和蛋白表达水平也对应降低(P <0.05)。肺腺癌组织Hck和EGFR mRNA的相对表达量均高于癌旁组织。Pearson相关性分析结果显示,癌组织中Hck mRNA与EGFR mRNA的表达呈正相关(r=0.555,P=0.017)。结论本研究发现Hck可能通过改变EGFR的表达水平调节肺腺癌细胞的生物学功能。

肿瘤坏死因子-α-转化酶和EGFR在非小细胞肺癌转移中的作用研究

目的探讨非小细胞肺癌(NSCLC)病理组织中肿瘤坏死因子-α-转化酶(TACE)和EGFR在原发灶和转移灶中的表达及其与患者预后的关系。方法应用液相芯片技术、RT-PCR、Western Blot等方法测定57例NSCLC和14例肺部良性病变病理切片中膜结合肿瘤坏死因子(M-TNF)、TACE、EGFR的水平,对比分析TACE、EGFR在NSCLC患者和正常人之间以及NSCLC原发灶和转移病灶的表达。结果 57例NSCLC中M-TNF和TACE的异常表达率分别为66.67%和64.91%,EGFR的阳性表达率为77.19%;14例肺部良性病变均未见TACE的过度表达;TACE和EGFR在NSCLC转移灶中的表达明显高于原发灶,并与预后成正相关。结论检测TACE和EGFR在NSCLC中的表达变化是判断恶性肿瘤程度、浸润转移的有效参考指标,TACE和EGFR的异常表达可能影响NSCLC患者的预后。