Eickelmann P, Ebert T, Warskulat U, Schulz W A, Sies H
Institut für Physiologische Chemie, Heinrich-Heine-Universität Düsseldorf, Germany.
Carcinogenesis. 1994 Feb;15(2):219-25. doi: 10.1093/carcin/15.2.219.
NAD(P)H:quinone oxidoreductase (NQOR) and glutathione S-transferases (GST) are enzymes of interest in cell defence and drug resistance. Relative levels of NQOR mRNA in renal cell carcinomas were 28 +/- 24% (n = 21) of those in non-neoplastic tissue and the enzyme activity decreased from 41 +/- 39 to 18 +/- 27 mU/mg protein (n = 23). In three of the cases, there was no measurable NQOR enzyme activity at all, indicating a polymorphism in the population for this gene. Relative GST-alpha mRNA levels in the tumours were on average 6 +/- 6% (n = 22) of the control value, whereas for GST-pi mRNA smaller decreases as well as increases were found in the tumours as compared to control tissue, but, on average, the level remained unchanged. Overall GST activity measured with CDNB as a substrate was 152 +/- 157 mU/mg protein in tumour tissue and 342 +/- 177 mU/mg protein in non-neoplastic tissue (n = 23). In all kidney tumour-derived cell lines NQOR mRNA was strongly expressed and on a per protein basis NQOR activity was about 10-fold higher than in the kidney tumour samples. GST-pi but not GST-alpha mRNA was also present. Total GST enzyme activities in these cell lines were similar to those in kidney tumour samples. HepG2 cells exhibited expression of NQOR and GST-alpha; GST-pi was not detectable. NQOR activity in HepG2 was about four-fold higher than in kidney-derived cell lines. Thus, NQOR and GST-alpha are both down-regulated in renal carcinoma, but their expression diverges in carcinoma cell lines.
NAD(P)H:醌氧化还原酶(NQOR)和谷胱甘肽S-转移酶(GST)是细胞防御和耐药性方面备受关注的酶。肾细胞癌中NQOR mRNA的相对水平为非肿瘤组织中的28±24%(n = 21),且酶活性从41±39降至18±27 mU/mg蛋白(n = 23)。在其中3例中,完全检测不到NQOR酶活性,表明该基因在人群中存在多态性。肿瘤中GST-α mRNA的相对水平平均为对照值的6±6%(n = 22),而与对照组织相比,肿瘤中GST-π mRNA既有较小程度的降低也有升高,但总体水平保持不变。以1-氯-2,4-二硝基苯(CDNB)为底物测得的肿瘤组织中总GST活性为152±157 mU/mg蛋白,非肿瘤组织中为342±177 mU/mg蛋白(n = 23)。在所有源自肾肿瘤的细胞系中,NQOR mRNA均强烈表达,且按蛋白计算,NQOR活性比肾肿瘤样本高约10倍。同时也存在GST-π mRNA,但不存在GST-α mRNA。这些细胞系中的总GST酶活性与肾肿瘤样本中的相似。HepG2细胞表达NQOR和GST-α;未检测到GST-π。HepG2中的NQOR活性比源自肾的细胞系高约4倍。因此,NQOR和GST-α在肾癌中均下调,但其在癌细胞系中的表达存在差异。
