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Monoamine oxidase A expression is suppressed in human cholangiocarcinoma via coordinated epigenetic and IL-6-driven events

机译:通过协调的表观遗传和IL-6驱动的事件,人胆管癌中单胺氧化酶A的表达受到抑制

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The secretion of dopamine and serotonin is increased in cholangiocarcinoma, which has growth-promoting effects. Monoamine oxidase A (MAOA), the degradation enzyme of serotonin and dopamine, is suppressed in cholangiocarcinoma via an unknown mechanism. The aims of this study were to (i) correlate MAOA immunoreactivity with pathophysiological parameters of cholangiocarcinoma, (ii) determine the mechanism by which MAOA expression is suppressed and (iii) evaluate the consequences of restored MAOA expression in cholangiocarcinoma. MAOA expression was assessed in cholangiocarcinoma and nonmalignant controls. The control of MAOA expression by promoter hypermethylation was evaluated and the contribution of interleukin-6 (IL-6) signaling to the suppression of MAOA expression was determined. The effects of MAOA overexpression on cholangiocarcinoma growth and invasion were also assessed. MAOA expression is correlated with differentiation, invasion and survival in cholangiocarcinoma. The MAOA promoter was hypermethylated immediately upstream of the start codon in cholangiocarcinoma samples and cell lines but not in nonmalignant counterparts. IL-6 signaling also decreased MAOA expression via a mechanism independent of hypermethylation, involving the regulation of the balance between SP-1 transcriptional activity and its inhibitor, R1 repressor. Inhibition of both IL-6 signaling and DNA methylation restored MAOA levels to those observed in cholangiocytes. Forced MAOA overexpression inhibited cholangiocarcinoma growth and invasion. MAOA expression is suppressed by the coordinated control of promoter hypermethylation and IL-6 signaling. MAOA may be a useful prognostic marker in the management of cholangiocarcinoma, and therapies designed to increase MAOA expression might prove beneficial in the treatment of cholangiocarcinoma.
机译:胆管癌中多巴胺和5-羟色胺的分泌增加,具有促进生长的作用。单胺氧化酶A(MAOA)是血清素和多巴胺的降解酶,在胆管癌中通过未知机制被抑制。这项研究的目的是(i)使MAOA免疫反应性与胆管癌的病理生理参数相关,(ii)确定抑制MAOA表达的机制,以及(iii)评估恢复的MAOA表达在胆管癌中的后果。在胆管癌和非恶性对照中评估了MAOA的表达。评估了通过启动子高甲基化对MAOA表达的控制,并确定了白介素6(IL-6)信号传导对抑制MAOA表达的作用。还评估了MAOA过表达对胆管癌生长和侵袭的影响。 MAOA的表达与胆管癌的分化,侵袭和生存有关。在胆管癌样品和细胞系中,MAOA启动子在起始密码子的上游立即被甲基化,而在非恶性对应物中则没有。 IL-6信号转导也通过不依赖于高甲基化的机制降低了MAOA表达,涉及调节SP-1转录活性与其抑制剂R1阻遏物之间的平衡。 IL-6信号传导和DNA甲基化的抑制将MAOA水平恢复为在胆管细胞中观察到的水平。强迫的MAOA过表达抑制胆管癌的生长和侵袭。通过协同控制启动子高甲基化和IL-6信号传导抑制了MAOA的表达。 MAOA在胆管癌的治疗中可能是有用的预后标志物,旨在提高MAOA表达的疗法可能在胆管癌的治疗中被证明是有益的。

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