Oxidative Metabolism Genes in Ovarian Neoplasms

E. Proskurnina, M. Fedorova, E. Savinova, V. I. Voznesenskii, S. Kostyuk, E. A. Sosnova
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Abstract

BACKGROUND: Reactive oxygen species play important and ambiguous role in carcinogenesis, and local oxidative metabolism may differ significantly from systemic metabolism and determine the processes occurring in tumor tissues. AIM: This study aimed to examine the expressions of key oxidative metabolism genes, particularly CYB5R, POR, NOX4, SOD1, NF-B, and NRF2, in ovarian neoplasm tissues, and determine cytochrome b5 reductase and cytochrome P450 reductase activity, blood neutrophil activity, and antioxidant indices in the blood plasma and peritoneal fluid. MATERIALS AND METHODS: The study included two groups of patients: a study group (n = 10) with ovarian adenocarcinoma and a comparison group (n = 6) with benign ovarian neoplasms. The expressions of CYB5R1, CYB5R2/R4, CYB5R3, POR, BIRC3, NOX4, NRF2, NF-B, SOD1, HMOX1, and BCL2 genes, cytochrome b5 reductase, and cytochrome P450 reductase activity, oxidative activity of blood neutrophils, and antioxidant potential of plasma and peritoneal fluid were evaluated in these two groups of women. RESULTS: The expression levels of CYB5R3 and BCL2 were significantly lower in adenocarcinoma tissues. The activities of cytochrome b5 reductase and cytochrome P450 reductase increased in the group with adenocarcinoma. On average, the activity of blood neutrophils corresponded to the reference values. For blood plasma, the antioxidant capacity were not different, whereas the antioxidant capacity in the peritoneal fluid increased approximately twofold in ovarian cancer. CONCLUSIONS: Significantly increased cytochrome b5 reductase activity in adenocarcinoma tissues may be a response to intracellular oxidative stress, whereas CYB5R3 gene expression may be reduced by a negative feedback mechanism. The activities of cytochrome P450 reductase and its gene change to a lesser extent in the presence of ovarian adenocarcinoma. The oxidative balance in the blood and peritoneal fluid correlated with the tissue expressions of NF-B and NRF2.
卵巢肿瘤中的氧化代谢基因
背景:活性氧在癌变过程中发挥着重要但不明确的作用,局部氧化代谢可能与全身代谢有很大不同,并决定了肿瘤组织中发生的过程。目的:本研究旨在检测卵巢肿瘤组织中CYB5R、POR、NOX4、SOD1、NF-B、NRF2等关键氧化代谢基因的表达,并测定血浆和腹膜液中细胞色素b5还原酶、细胞色素P450还原酶活性、血液中性粒细胞活性及抗氧化指标。材料与方法:该研究包括两组患者:研究组(n = 10)患有卵巢腺癌,对照组(n = 6)患有良性卵巢肿瘤。检测两组妇女的CYB5R1、CYB5R2/R4、CYB5R3、POR、BIRC3、NOX4、NRF2、NF-B、SOD1、HMOX1、BCL2基因表达、细胞色素b5还原酶、细胞色素P450还原酶活性、血液中性粒细胞氧化活性、血浆和腹膜液抗氧化电位。结果:CYB5R3和BCL2在腺癌组织中的表达水平明显降低。腺癌组细胞色素b5还原酶和细胞色素P450还原酶活性升高。平均而言,血液中性粒细胞的活性与参考值相符。血浆的抗氧化能力没有差异,而卵巢癌患者腹膜液的抗氧化能力增加了约两倍。结论:腺癌组织中细胞色素b5还原酶活性的显著升高可能是对细胞内氧化应激的反应,而CYB5R3基因表达的降低可能是一种负反馈机制。卵巢腺癌患者细胞色素P450还原酶活性及其基因变化较小。血液和腹膜液中的氧化平衡与组织中NF-B和NRF2的表达相关。
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