首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Use of monoclonal antibodies to keratin 7 in the differential diagnosis of adenocarcinomas.
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Use of monoclonal antibodies to keratin 7 in the differential diagnosis of adenocarcinomas.

机译:抗角蛋白7单克隆抗体在腺癌的鉴别诊断中的应用。

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摘要

Monoclonal antibodies (MAbs) to specific keratin subtypes were prepared and characterized by immunoblotting and immunohistochemical assays on human cell cultures and normal and malignant human tissues. Chain-specific MAbs to keratin 7 (RCK 105, OV-TL 12/30) and keratin 18 (RGE 53, RCK 106, CK18-2), as well as broadly cross-reacting keratin MAbs (RCK 102, OV-TL 12/5) could be shown to react with different types of human epithelial tissues and were therefore tested for their usefulness in the differential diagnosis of carcinomas. The two broad-spectrum antibodies stained virtually all of the more than 350 carcinomas tested, especially when combined, and distinguished them from most nonepithelial tumors. The keratin 18 MAbs distinguished adenocarcinomas (which are keratin 18 positive) from most squamous cell carcinomas (which are generally keratin 18 negative). The MAbs to keratin 7 could be shown to recognize specific subtypes of adenocarcinoma and could, for example, distinguish between ovarian carcinomas (keratin 7 positive) and carcinomas of the gastrointestinal tract (keratin 7 negative), or between transitional cell carcinomas (keratin 7 positive) and prostate cancer (keratin 7 negative). In general, malignancies showed the expected keratin reactivity pattern as concluded from the keratin pattern of its cell of origin or its type of differentiation. The use of an extended series of malignancies did, however, also illustrate that exceptions to this rule exist. For example, certain antibodies to keratin 18 stained tumor areas in squamous cell carcinomas of the lung. Also a certain percentage of tumors, which generally showed no keratin 7 expression, were positive with RCK 105 or OV-TL 12/30. On the other hand, a certain percentage of tumors, which were generally positive for keratin 7, did not show a staining reaction with these MAbs. Furthermore subtle differences between reactivity patterns of different MAbs recognizing the same keratin protein were observed, both in the normal and malignant human tissues, indicating that specific keratin epitopes may be masked in certain tissues and that unmasking of such epitopes can occur with malignant progression. This phenomenon may be of some use in a further subtyping of carcinomas, especially those of the gastrointestinal tract. Despite these exceptional staining patterns, the keratin MAbs described above have proved to be useful tools in the characterization of epithelial tumors in routine histopathology and cytopathology, in which they add to a more refined diagnosis of (adeno)carcinomas.
机译:制备了针对特定角蛋白亚型的单克隆抗体(MAb),并通过在人体细胞培养物以及正常和恶性人体组织上的免疫印迹和免疫组化分析进行了表征。角蛋白7(RCK 105,OV-TL 12/30)和角蛋白18(RGE 53,RCK 106,CK18-2)的链特异性单克隆抗体,以及广泛交叉反应的角蛋白MAb(RCK 102,OV-TL 12 / 5)可能与不同类型的人类上皮组织发生反应,因此测试了它们在癌症鉴别诊断中的作用。两种广谱抗体几乎对所有超过350种癌症进行了染色,尤其是组合使用时,它们与大多数非上皮性肿瘤区分开来。角蛋白18 MAb与大多数鳞状细胞癌(通常是角蛋白18阴性)区分开来的腺癌(角蛋白18阳性)。可以证明角蛋白7的单克隆抗体可以识别腺癌的特定亚型,并且可以例如区分卵巢癌(角蛋白7阳性)和胃肠道癌(角蛋白7阴性)或移行细胞癌(角蛋白7阳性)。 )和前列腺癌(角蛋白7阴性)。通常,恶性肿瘤显示出预期的角蛋白反应性模式,这是由其起源细胞或分化类型的角蛋白模式得出的。但是,使用一系列扩展的恶性肿瘤确实说明了该规则的例外。例如,肺鳞状细胞癌中某些针对角蛋白18的抗体染色了肿瘤区域。同样,一定比例的肿瘤(通常不显示角蛋白7表达)在RCK 105或OV-TL 12/30中呈阳性。另一方面,通常对角蛋白7呈阳性的一定比例的肿瘤未显示出与这些MAb的染色反应。此外,在正常和恶性人类组织中均观察到识别相同角蛋白的不同单克隆抗体反应模式之间的细微差异,这表明特定的角蛋白表位可能在某些组织中被掩盖,并且这种表位的不掩盖可能随着恶性进展而发生。这种现象可能在进一步的癌亚型,尤其是胃肠道癌的亚型中有用。尽管有这些异常的染色模式,但上述角蛋白单抗已被证明是常规组织病理学和细胞病理学中表征上皮肿瘤的有用工具,在这些特征中,它们可加深对(腺)癌的诊断。

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