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首页> 外文期刊>BMC Pulmonary Medicine >Knockdown of circ-ABCB10 promotes sensitivity of lung cancer cells to cisplatin via miR-556-3p/AK4 axis
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Knockdown of circ-ABCB10 promotes sensitivity of lung cancer cells to cisplatin via miR-556-3p/AK4 axis

机译:Circ-ABCB10的敲低通过MIR-556-3P / AK4轴促进肺癌细胞对顺铂的敏感性

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Due to the acquired drug resistance, the potency of cisplatin-based chemotherapy is limited in lung cancer, which is a big obstacle in clinical treatment of lung cancer. Abundant evidence has revealed that circular RNAs (circRNAs) exerted facilitating or suppressive function on the tumorigenesis of multiple cancers. The oncogenic role of circ-ABCB10 in breast cancer and clear cell renal cell carcinoma has been validated in recent researches. However, the regulatory mechanism of circ-ABCB10 and its relation to cellular sensitivity to cisplatin in lung cancer is poorly understood. The expression and characteristic of circ-ABCB10 were analyzed by RT-qPCR and nucleic acid electrophoresis. CCK-8, colony formation, TUNEL and transwell assays were applied to probe the role of FOXD3-AS1 in lung cancer. The interactions of miR-556-3p with circ-ABCB10 and AK4 were testified by luciferase reporter and RIP assays. Circ-ABCB10 was markedly upregulated and featured with loop structure in lung cancer. Circ-ABCB10 depletion suppresses lung cancer progression and sensitizes lung cancer cells to cisplatin. Molecular mechanism assays manifested that circ-ABCB10 bound with miR-556-3p and negatively modulated miR-556-3p expression. Additionally, AK4 was testified to be the downstream target of miR-556-3p. More importantly, rescue assays clarified that upregulation of AK4 could reverse the cisplatin-sensitizing and tumor-suppressing effect of circ-ABCB10 knockdown on lung cancer cells. Circ-ABCB10 knockdown enhances sensitivity of lung cancer cells to cisplatin by targeting miR-556-3p/AK4 axis.
机译:由于获得的耐药性,顺铂的化疗效力是肺癌的有限,这是肺癌临床治疗的一个大障碍。丰富的证据表明,循环RNA(CircRNA)施加促进或抑制多种癌症的肿瘤内疾病的功能。近期研究验证了乳腺癌和透明细胞肾细胞癌的Circ-ABCB10在乳腺癌和透明细胞肾细胞癌中的致癌作用。然而,Circ-ABCB10的监管机制及其与肺癌中顺铂的细胞敏感性的关系较差。通过RT-QPCR和核酸电泳分析循环ABCB10的表达和特征。 CCK-8,菌落形成,Tunel和Transwell测定探讨了Foxd3-AS1在肺癌中的作用。用荧光素酶报告者和RIP测定法妥化MiR-556-3P与循环ABCB10和AK4的相互作用。 Circ-ABCB10明显上调,并以肺癌环状结构为特色。 Circ-ABCB10耗竭抑制肺癌进展,并使肺癌细胞敏感到顺铂。分子机制测定表现出循环ABCB10与miR-556-3p结合并对miR-556-3p表达结合。另外,AK4被证明是miR-556-3p的下游靶标。更重要的是,救援分析澄清了AK4的上调可以逆转CiSplatin敏化和肿瘤抑制效应肺癌细胞对肺癌细胞的影响。 Circ-ABCB10通过靶向miR-556-3p / ak4轴来增强肺癌细胞对顺铂的敏感性。

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