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NMDA receptors are expressed in human ovarian cancer tissues and human ovarian cancer cell lines

机译:NMDA受体在人卵巢癌组织和人卵巢癌细胞系中表达

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摘要

We have earlier demonstrated that breast cancer and small-cell lung cancer express functional NMDA receptors that can be targeted to promote cancer cell death. Human ovarian cancer tissues and human ovarian cancer cell lines (SKOV3, A2008, and A2780) have now been shown to also express NMDA-receptor subunit 1 (GluN1) and subunit 2B (GluN2B). Seventeen ovarian cancers in two arrays were screened by immunohistochemistry using polyclonal antibodies that recognize an extracellular moiety on GluN1 and on GluN2B. These specimens comprised malignant tissue with pathology diagnoses of serous papillary cystadenocarcinoma, endometrioid adenocarcinoma, and clear-cell carcinoma. Additionally, archival tissues defined as ovarian adenocarcinoma from ten patients treated at this institute were also evaluated. All of the cancerous tissues demonstrated positive staining patterns with the NMDA-receptor antibodies, while no staining was found for tumor-adjacent normal tissues or sections of normal ovarian tissue. Human ovarian adenocarcinoma cell lines (A2008, A2780, SKOV3) were demonstrated to express GluN1 by Western blotting, but displayed different levels of expression. Through immunocytochemistry utilizing GluN1 antibodies and imaging using a confocal microscope, we were able to demonstrate that GluN1 protein is expressed on the surface of these cells. In addition to these findings, GluN2B protein was demonstrated to be expressed using polyclonal antibodies against this protein. Treatment of all ovarian cell lines with antibodies against GluN1 was found to result in decreased cell viability (P<0.001), with decreases to 10%–25% that of untreated cells. Treatment of control HEK293 cells with various dilutions of GluN1 antibodies had no effect on cell viability. The GluN1 antagonist MK-801 (dizocilpine maleate) and the GluN2B antagonist ifenprodil, like antibodies, dramatically decreased the viability of A2780 ovarian tumor cells (P<0.01). Treatment of A2780 tumor xenografts with ifenprodil (2.5 mg/kg body weight/day) significantly reduced tumor growth in nuu mice. Our findings suggest that both GluN1 and GluN2B proteins as membrane components could be readily available targets for the treatment of most ovarian cancers.
机译:我们较早的研究表明,乳腺癌和小细胞肺癌表达的功能性NMDA受体可以靶向促进癌细胞死亡。现在已显示人类卵巢癌组织和人类卵巢癌细胞系(SKOV3,A2008和A2780)还表达NMDA受体亚基1(GluN1)和亚基2B(GluN2B)。使用识别GluN1和GluN2B上细胞外部分的多克隆抗体,通过免疫组织化学筛选了两个阵列中的17个卵巢癌。这些标本包括具有浆液性乳头状膀胱腺癌,子宫内膜样腺癌和透明细胞癌的病理诊断的恶性组织。此外,还评估了在该研究所接受治疗的十名患者的定义为卵巢腺癌的档案组织。所有癌变组织均显示NMDA受体抗体呈阳性染色模式,而与肿瘤相邻的正常组织或正常卵巢组织切片未发现染色。人类卵巢腺癌细胞系(A2008,A2780,SKOV3)已通过蛋白质印迹法表达GluN1,但表现出不同的表达水平。通过利用GluN1抗体的免疫细胞化学和共聚焦显微镜成像,我们能够证明GluN1蛋白在这些细胞的表面表达。除了这些发现,GluN2B蛋白被证明是使用针对该蛋白的多克隆抗体表达的。发现用抗GluN1抗体处理所有卵巢细胞系会导致细胞活力降低(P <0.001),降至未处理细胞的10%–25%。用各种稀释的GluN1抗体处理对照HEK293细胞对细胞生存力没有影响。 GluN1拮抗剂MK-801(马来酸二唑西平)和GluN2B拮抗剂ifenprodil像抗体一样,显着降低了A2780卵巢肿瘤细胞的活力(P <0.01)。用艾芬洛地尔(2.5 mg / kg体重/天)治疗A2780肿瘤异种移植物可显着降低nu / nu小鼠的肿瘤生长。我们的发现表明,作为膜成分的GluN1和GluN2B蛋白都可以很容易地用于治疗大多数卵巢癌。

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