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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Increased local dopamine secretion has growth-promoting effects in cholangiocarcinoma.
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Increased local dopamine secretion has growth-promoting effects in cholangiocarcinoma.

机译:在胆管癌中,局部多巴胺分泌的增加具有促进生长的作用。

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摘要

Cholangiocarcinoma is a devastating cancer of biliary origin with limited treatment options. Symptoms are usually evident after blockage of the bile duct by the tumor, and at this late stage, they are relatively resistant to chemotherapy and radiation therapy. Therefore, it is imperative that alternative treatment options are explored. We have previously shown that serotonin metabolism is dysregulated in cholangiocarcinoma leading to an increased secretion of serotonin, which has growth-promoting effects. Because serotonin and dopamine share the degradation machinery, we evaluated the secretion of dopamine from cholangiocarcinoma and its effects on cell proliferation. Using 4 cholangiocarcinoma cell lines and human biopsy samples, we demonstrated that there was an increase in mRNA and protein expression of the dopamine synthesis enzymes tyrosine hydroxylase and dopa decarboxylase in cholangiocarcinoma. There was increased dopamine secretion from cholangiocarcinoma cell lines compared to H69 and HIBEC cholangiocytes and increased dopamine immunoreactivity in human biopsy samples. Furthermore, administration of dopamine to all cholangiocarcinoma cell lines studied increased proliferation by up to 30%, which could be blocked by the pretreatment of the D2 and D4 dopamine receptor antagonists, whereas blocking dopamine production by alpha-methyldopa administration suppressed growth by up to 25%. Administration of alpha-methyldopa to nude mice also suppressed cholangiocarcinoma tumor growth. The data presented here represent the first evidence that dopamine metabolism is dysregulated in cholangiocarcinoma and that modulation of dopamine synthesis may represent an alternative target for the development of therapeutic strategies.
机译:胆管癌是一种破坏性胆源性癌症,治疗选择有限。症状通常在肿瘤阻塞胆管后出现,并且在此晚期,它们对化学疗法和放射疗法有相对的抵抗力。因此,必须探索替代治疗方案。先前我们已经表明,胆管癌中5-羟色胺的代谢失调,导致5-羟色胺分泌增加,这具有促进生长的作用。由于5-羟色胺和多巴胺具有降解机制,因此我们评估了胆管癌中多巴胺的分泌及其对细胞增殖的影响。使用4种胆管癌细胞系和人体活检样本,我们证明了胆管癌中多巴胺合成酶酪氨酸羟化酶和多巴脱羧酶的mRNA和蛋白表达增加。与H69和HIBEC胆管细胞相比,胆管癌细胞系中多巴胺的分泌增加,人活检样品中的多巴胺免疫反应性增加。此外,向所有研究的胆管癌细胞系施用多巴胺可将增殖最多增加30%,这可以通过D2和D4多巴胺受体拮抗剂的预处理来阻止,而通过α-甲基多巴施用来阻止多巴胺的产生则最多可抑制25%的生长。 %。给裸鼠施用α-甲基多巴也抑制了胆管癌肿瘤的生长。此处提供的数据代表胆管癌中多巴胺代谢失调的第一个证据,而多巴胺合成的调节可能代表治疗策略发展的另一目标。

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