Estrogen Sulfotransferase (SULT1E1) and NFκβ Confer Matrix Metalloprotease (MMP 2/9) Action in Breast Carcinogenesis

被引:0
作者
Nazmeen, Aarifa [1 ]
Maiti, Sayantani [1 ]
Ghosh, Tamal Kanti [2 ]
Maiti, Smarajit [1 ,3 ,4 ]
机构
[1] OIST, Dept Biochem & Biotechnol, Cell & Mol Therapeut Lab, Midnapore 721102, India
[2] Deben Mahata Govt Med Coll & Hosp, Purulia 723147, West Bengal, India
[3] Haldia Inst Hlth Sci, ICARE Complex,Hatiberia,Purba Medinipur, Haldia 721657, West Bengal, India
[4] Agricure Biotech Res Soc, Midnapore 721101, West Bengal, India
关键词
Estrogen; Breast cancer; Oxidant stress; Nrf2; NF kappa beta; Triad function; SIGNALING PATHWAYS; OXIDATIVE STRESS; CANCER CELLS; EXPRESSION; GROWTH; DEXAMETHASONE; INHIBITION; INVASION;
D O I
10.1007/s40944-024-00925-7
中图分类号
R71 [妇产科学];
学科分类号
100211 ;
摘要
BackgroundEstrogen (E2) is a signaling molecule that controls cell differentiation/early embryogenesis/organogenesis. Nevertheless, during adolescence/adulthood it influences female reproductive functions via nongenomic (cellular signaling)/genomic (transcriptional signaling) pathways by recruiting a number of genes/proteins.ObjectivesIn postmenopausal women, increased E2 causes malignancies in the breast and gynecologic tissues. An aberrant redox control of the estrogen-metabolizing enzyme like estrogen sulfotransferase (SULT1E1), transcription factors NF kappa beta/Nrf2, and matrix metalloproteases (MMP 2/9) results in impaired estrogenic signaling.MethodsHere, the tumor and its surrounding tissues underwent a redox-state screening. In rat liver tissues treated with lansoprazole (Nrf2 inducer) and dexamethasone (SULT1E1 inducer), RT-PCR was performed to measure SULT1E1 expression in human breast cancer tissues and the MMP 2/9 activities by gel zymogram technique. Using immunohistochemistry, the location of SULT1E1/NF kappa beta was examined.ResultsExtensive protein-protein interactions (MMP2/9 and Nrf2) were studied by the STRING Bioinformatics software to characterize metabolic functional dependence. It can be hypothesized transcription factors (NF kappa beta/Nrf2) influence MMP expressions, which has a major impact on the metastatic transformation of breast cancer. Breast cancers exhibit elevated Nrf2/NF kappa B/SULT1E1 expression and immunolocalization. Lansoprazole and dexamethasone both demonstrated antioxidant induction by increasing catalase and SOD activities and Nrf2 protein expressions. Statistical implications strongly justify correlations among SULT1E1 and Nrf2 inductions also with antioxidant enzymes. Canonical correlation, multiple comparisons Dunnett's, and ANOVA test support these statistics. The relation between Nrf2/NF kappa B is determined by the oxidative stress and MMP-dependent cellular/transcriptional regulations of other biomolecules. Moreover, SULT1E1-mediated E2 levels and MMP functions are determined by this relationship.ConclusionsThe role of MMPs in the severity of human breast carcinogenesis is thought to be carried out by the regulation of NF kappa beta, SULTN1E1, and Nrf2. This regulatory system may be therapeutically targeted to treat breast cancer.
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页数:13
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