抗谷氨酸受体2作为前列腺癌新的潜在诊断探针:免疫组化初步研究

Jaclyn F Hechtman, Guang Q Xiao, Pamela D Unger, Yayoi Kinoshita, James H Godbold, David E Burstein
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引用次数: 0

摘要

前列腺癌(PC)的诊断随着广泛的筛查而增加。虽然使用α-甲基辅酶a消旋酶和高分子量细胞角蛋白有助于区分良性模拟和恶性肿瘤,但其敏感性和特异性是有限的。我们研究了6C4,一种针对谷氨酸受体2的单克隆抗体,谷氨酸受体2是一种分布于整个中枢神经系统的兴奋性氨基酸受体亚基,在良性前列腺上皮、高级别前列腺上皮内瘤变和PC中的作用。10例萎缩后或腺病样前列腺也被染色为前列腺上皮内瘤变4,这是一种针对α-甲基酰基辅酶a消旋酶、p63和高分子量细胞角蛋白的鸡尾酒免疫染色,与6C4平行。6C4的免疫反应性分为阴性(0% ~ 10%)、+1(11% ~ 50%)和+2(50%)。恶性上皮按Gleason模式分类。Gleason型4和5分为筛网型和非筛网型。它在区分前列腺癌(前列腺上皮内瘤变4免疫染色均显示基底细胞缺失)和前列腺后营养或腺样腺的作用也进行了研究。我们的结果显示在良性分泌性前列腺上皮、高级别前列腺上皮内瘤变和低格里森型癌的染色上有统计学上的显著差异。结果还表明,6C4是区分前列腺癌基底细胞阴性后营养或腺样腺的敏感标志物。此外,筛状与非筛状Gleason 4型和5型癌的染色差异有统计学意义。我们研究了有限数量的筛状癌和非筛状癌的淋巴结转移,在大多数病例中,它们的染色与原发肿瘤相同。总之,我们的初步数据显示了6C4在PC病理评估中的潜在效用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Anti-glutamate receptor 2 as a new potential diagnostic probe for prostatic adenocarcinoma: a pilot immunohistochemical study.

Diagnoses of prostatic carcinoma (PC) have increased with widespread screening. While the use of α-methylacyl coA racemase and high molecular weight cytokeratins have aided in distinguishing benign mimics from malignancy, their sensitivity and specificity are limited. We studied 6C4, a monoclonal antibody to glutamate receptor 2, an excitatory amino acid receptor subunit distributed throughout the central nervous system, on benign prostatic epithelium, high-grade prostatic intraepithelial neoplasia, and PC. Ten cases with post-atrophic or adenosis-like prostate glands were also stained with prostatic intraepithelial neoplasia 4, an immunostain cocktail against α-methylacyl coA racemase, p63, and high molecular weight cytokeratin, in parallel with 6C4. Immunoreactivity for 6C4 was graded as negative (0% to 10%), +1 (11%% to 50%), and +2 (>50%). Malignant epithelium was classified by Gleason patterns. Gleason patterns 4 and 5 were subdivided into cribriform or noncribriform type. Its utility in distinguishing postatrophic or adenosis-like glands from prostate cancer, both of which show absence of basal cells on prostatic intraepithelial neoplasia 4 immunostain, was also investigated. Our results revealed a statistically significant difference in staining of benign secretory prostatic epithelium, high-grade prostatic intraepithelial neoplasia, and low Gleason pattern carcinomas. The results also showed 6C4 is a sensitive marker in separating basal cell negative postatrophic or adenosis-like glands from prostate carcinoma. In addition, there was a statistically significant difference between staining of cribriform versus noncribriform Gleason pattern 4 and 5 carcinomas. A limited number of lymph node metastases from cribriform and noncribriform carcinomas were studied, and they stained the same as the primary tumor in the majority of cases. In conclusion, our preliminary data demonstrated potential utility of 6C4 in the pathologic evaluation of PC.

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