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Human glandular kallikrein 2 expression in prostate adenocarcinoma and lymph node metastases.

机译:人腺激肽释放酶2在前列腺腺癌和淋巴结转移中的表达。

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OBJECTIVES: To describe the expression of a potential new tumor marker, human glandular kallikrein 2 (hK2), in primary adenocarcinoma and lymph node metastases that may be useful as an adjunct to prostate-specific antigen (PSA) in the diagnosis and monitoring of prostate cancer. METHODS: We evaluated 151 radical prostatectomy specimens removed at Mayo Clinic with node-positive adenocarcinoma to compare cytoplasmic expression of hK2, pro-hK2, and PSA in benign tissue, prostate adenocarcinoma, and lymph node metastases. Monoclonal antibodies for mature hK2 (hK2-G586), pro-hK2 (pro-hK2-G464), and PSA (PSA-773) were used. A polyclonal antibody for PSA was also used. Immunoreactivity in each case was tested to determine whether cancer recurrence could be predicted. RESULTS: Intense epithelial cytoplasmic immunoreactivity was observed in every case for hK2-G586, pro-hK2-G464, PSA-773, and polyclonal PSA (100% of cases, respectively). The intensity and extent of hK2 expression was greater in lymph node metastases than in primary cancer; furthermore, the expression in primary cancer was greater than in benign epithelium. Pro-hK2 was expressed in a greater percentage of cells in primary cancer than in benign tissue; furthermore, pro-hK2 was expressed to a greater extent in primary cancer than in lymph node metastases. In marked contrast to mature hK2, monoclonal PSA immunoreactivity was expressed to a higher extent in primary cancer than in lymph node metastases. Polyclonal PSA showed an incremental increase in expression from benign tissue to primary cancer and a further increase in expression in lymph node metastases. CONCLUSIONS: hK2 was expressed in every cancer, and the expression incrementally increased from benign epithelium to primary cancer and lymph node metastases. Pro-hK2 was expressed to the greatest extent in primary cancer. Monoclonal PSA displayed inverse immunoreactivity compared with hK2. Polyclonal PSA showed incremental increases, suggesting that both hK2 and PSA were being detected. Tissue expression of hK2 appears to be regulated independently of PSA in benign epithelium, adenocarcinoma, and lymph node metastases.
机译:目的:描述潜在的新型肿瘤标志物,人腺激肽释放酶2(hK2)在原发性腺癌和淋巴结转移中的表达,这些前列腺癌可作为前列腺特异性抗原(PSA)的辅助物用于诊断和监测前列腺癌症。方法:我们评估了梅奥诊所切除的151例淋巴结阳性腺癌根治性前列腺切除术标本,以比较hK2,pro-hK2和PSA在良性组织,前列腺腺癌和淋巴结转移中的胞浆表达。使用了成熟的hK2(hK2-G586),pro-hK2(pro-hK2-G464)和PSA(PSA-773)的单克隆抗体。还使用了PSA的多克隆抗体。测试每种情况下的免疫反应性,以确定是否可以预测癌症复发。结果:在每种情况下,hK2-G586,pro-hK2-G464,PSA-773和多克隆PSA均观察到强烈的上皮细胞质免疫反应(分别为100%的病例)。淋巴结转移中hK2表达的强度和程度要高于原发癌。此外,原发癌中的表达高于良性上皮中的表达。原发癌中Pro-hK2在细胞中的表达高于良性组织。此外,原发性癌中前hK2的表达程度高于淋巴结转移。与成熟的hK2形成鲜明对比的是,在原发癌中比在淋巴结转移中表达更高的单克隆PSA免疫反应性。多克隆PSA显示从良性组织到原发癌的表达增加,而在淋巴结转移中的表达进一步增加。结论:hK2在每种癌症中都有表达,并且表达从良性上皮到原发癌和淋巴结转移都逐渐增加。 Pro-hK2在原发性癌症中得到最大程度的表达。与hK2相比,单克隆PSA显示出反向的免疫反应性。多克隆PSA显示增加,表明同时检测到hK2和PSA。 hK2的组织表达似乎在良性上皮,腺癌和淋巴结转移中独立于PSA受到调节。

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