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Case 1: Raccoon eyes in an 8-month-old infant: Case 1 discussion

机译:案例1:8个月大婴儿的浣熊眼睛:案例1讨论

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d-glucuronyl C5-epimerase (GLCE) is involved in breast and lung carcinogenesis as a potential tumor suppressor gene, acting through inhibition of tumor angiogenesis and invasion/metastasis pathways. However, in prostate tumors, increased GLCE expression is associated with advanced disease, suggesting versatile effects of GLCE in different cancers. To investigate further the potential cancer-promoting effect of GLCE in prostate cancer, GLCE was ectopically re-expressed in morphologically different LNCaP and PC3 prostate cancer cells. Transcriptional profiles of normal PNT2 prostate cells, LNCaP, PC3 and DU145 prostate cancer cells, and GLCE-expressing LNCaP and PC3 cells were determined. Comparative analysis revealed the genes whose expression was changed in prostate cancer cells compared with normal PNT2 cells, and those differently expressed between the cancer cell lines (ACTA2, IL6, SERPINE1, TAGLN, SEMA3A, and CDH2). GLCE re-expression influenced mainly angiogenesis-involved genes (ANGPT1, SERPINE1, IGF1, PDGFB, TNF, IL8, TEK, IFNA1, and IFNB1) but in a cell type-specific manner (from basic deregulation of angiogenesis in LNCaP cells to significant activation in PC3 cells). Invasion/metastasis pathway was also affected (MMP1, MMP2, MMP9, S100A4, ITGA1, ITGB3, ERBB2, and FAS). The obtained results suggest activation of angiogenesis as a main molecular mechanism of pro-oncogenic effect of GLCE in prostate cancer. GLCE up-regulation plus expression pattern of a panel of six genes, discriminating morphologically different prostate cancer cell sub-types, is suggested as a potential marker of aggressive prostate cancer.
机译:d-葡萄糖醛酸酰基C5-表异构酶(GLCE)作为潜在的抑癌基因参与乳腺癌和肺癌的发生,通过抑制肿瘤血管生成和侵袭/转移途径发挥作用。但是,在前列腺肿瘤中,GLCE表达的增加与晚期疾病有关,这表明GLCE在不同癌症中具有多种作用。为了进一步研究GLCE在前列腺癌中的潜在促癌作用,GLCE在形态上不同的LNCaP和PC3前列腺癌细胞中异位重新表达。确定了正常PNT2前列腺细胞,LNCaP,PC3和DU145前列腺癌细胞以及表达GLCE的LNCaP和PC3细胞的转录谱。对比分析显示,与正常的PNT2细胞相比,在前列腺癌细胞中表达发生改变的基因,以及在癌细胞系之间表达不同的基因(ACTA2,IL6,SERPINE1,TAGLN,SEMA3A和CDH2)。 GLCE重新表达主要影响涉及血管生成的基因(ANGPT1,SERPINE1,IGF1,PDGFB,TNF,IL8,TEK,IFNA1和IFNB1),但以细胞类型特异性方式(从LNCaP细胞中血管生成的基本失调到显着激活)在PC3单元中)。入侵/转移途径也受到影响(MMP1,MMP2,MMP9,S100A4,ITGA1,ITGB3,ERBB2和FAS)。获得的结果表明,血管生成的活化是GLCE在前列腺癌中促癌作用的主要分子机制。 GLCE上调加上一组六个基因的表达模式,可以区分形态不同的前列腺癌细胞亚型,被认为是侵袭性前列腺癌的潜在标志。

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