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首页> 外文期刊>Cancer biology & therapy >Oxygenation inhibits ovarian tumor growth by downregulating STAT3 and cyclin-D1 expressions.
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Oxygenation inhibits ovarian tumor growth by downregulating STAT3 and cyclin-D1 expressions.

机译:氧合通过下调STAT3和cyclin-D1表达来抑制卵巢肿瘤的生长。

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Hypoxia, which is commonly observed in many solid tumors, is a major impediment to chemo- or radiation therapy. Hypoxia is also known to overexpress/activate signal transducer and activator of transcription 3 (STAT3) leading to tumor progression as well as drug resistance. We hypothesized that increased oxygenation of the hypoxic tumor may have an inhibitory effect on STAT3 activation and hence tumor-growth inhibition. Mice containing human ovarian cancer xenograft tumor were exposed to hyperbaric oxygen (HBO; 100% oxygen; 2 atm; 90-min duration) daily, for up to 21 days. Mice exposed to HBO showed a significant reduction in tumor volume, with no effect on body weight. STAT3 (Tyr 705) activation and cyclin-D1 protein/mRNA levels were significantly decreased up on HBO exposure. Interestingly, HBO exposure, in combination with weekly administration of cisplatin, also significantly reduced the tumor volume; however, this group of mice had drastically reduced body weight when compared to other groups. While conventional wisdom might suggest that increased oxygenation of tumors would promote tumor growth, the results of the present study indicated otherwise. Hyperoxia appears to inhibit STAT3 activation, which is a key step in the ovarian tumor progression. The study may have important implications for the treatment of ovarian cancer in the clinic.
机译:在许多实体瘤中普遍观察到的缺氧是化学疗法或放射疗法的主要障碍。缺氧还已知过表达/激活信号转导子和转录激活子3(STAT3),导致肿瘤进展以及耐药性。我们假设缺氧肿瘤的氧合增加可能对STAT3激活具有抑制作用,因此对肿瘤生长具有抑制作用。每天将含有人类卵巢癌异种移植肿瘤的小鼠暴露于高压氧(HBO; 100%氧气; 2个大气压;持续时间为90分钟),最多21天。暴露于HBO的小鼠显示肿瘤体积显着减少,对体重没有影响。 STAT3(Tyr 705)激活和细胞周期蛋白D1蛋白/ mRNA水平在HBO暴露下显着降低。有趣的是,HBO暴露与每周一次顺铂给药相结合,也可显着减少肿瘤体积。但是,与其他组相比,该组小鼠的体重显着降低。尽管传统观点可能暗示增加肿瘤的氧合将促进肿瘤的生长,但本研究的结果表明并非如此。高氧似乎抑制STAT3激活,这是卵巢肿瘤进展的关键步骤。该研究可能对临床治疗卵巢癌具有重要意义。

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