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Immunological Quantitation of DT‐Diaphorase in Carcinoma Cell Lines and Clinical Colon Cancers: Advanced Tumors Express Greater Levels of DT‐Diaphorase

机译:癌细胞系和临床结肠癌中DT-黄递酶的免疫定量:晚期肿瘤表达更高水平的DT-黄递酶

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摘要

NAD(P)H:quinone oxidoreductase (DT‐diaphorase; DTD) plays a major role in activating mitomycin C (MMC) in human colon and gastric carcinoma cell lines. Thus, measurement of DTD in clinical tumor samples could be beneficial in designing adjuvant chemotherapy. We explored immunological quantitation of DTD protein using a monoclonal antibody against DTD, demonstrating a close correlation between protein expression and enzyme activity of DTD in colon and gastric carcinoma cell lines and in colorectal tumor samples. This indicates that such immunoblot analysis is a simple alternative method for quantitating DTD in clinically excised samples. In most colorectal tumor samples, the tumors expressed larger amounts of DTD than did the peripheral normal tissues, suggesting a selective toxicity of MMC toward tumor cells. Also tumors with nodal metastases showed significantly higher DTD levels than did tumors without metastasis. These results raise the possibility that DTD expression is related to tumorigenesis and malignant progression of colorectal tumors. Measurement of DTD by the immunological method described here could be beneficial in designing a rational adjuvant chemotherapy with MMC.
机译:NAD(P)H:醌氧化还原酶(DT-diaphorase; DTD)在激活人结肠癌和胃癌细胞系中的丝裂霉素C(MMC)中起主要作用。因此,测量临床肿瘤样品中的DTD可能有助于设计辅助化疗。我们探索了针对DTD的单克隆抗体对DTD蛋白的免疫定量分析,证明了在结肠癌和胃癌细胞系以及结直肠肿瘤样品中DTD的蛋白表达与酶活性之间有着密切的关系。这表明这种免疫印迹分析是定量临床切除样品中DTD的简单替代方法。在大多数结直肠肿瘤样品中,肿瘤表达的DTD量大于周围正常组织,这表明MMC对肿瘤细胞具有选择性毒性。同样,具有淋巴结转移的肿瘤比无转移的肿瘤显示出更高的DTD水平。这些结果增加了DTD表达与大肠肿瘤的肿瘤发生和恶性进展相关的可能性。通过此处描述的免疫学方法对DTD的测量可能有助于设计合理的MMC辅助化疗。

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