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MEK 抑制诱导实验性肝细胞癌中 MRP1 和 MRP3 表达下调。

MEK inhibition induced downregulation of MRP1 and MRP3 expression in experimental hepatocellular carcinoma.

机构信息

Department of General and Transplant Surgery, Ruprecht-Karls-University, Im Neuenheimer Feld 110, Heidelberg, 69120, Germany.

Department of Breast Surgery, Xiangya Hospital, Zhongnan University, Changsha, 410008, China.

出版信息

Cancer Cell Int. 2013 Jan 15;13(1):3. doi: 10.1186/1475-2867-13-3.

DOI:10.1186/1475-2867-13-3

PMID:23320839

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3558388/

Abstract

BACKGROUND

Hepatocellular carcinoma (HCC) exhibits strong intrinsic and acquired drug resistance which is the main obstacle to chemotherapy. Overexpression of ATP binding cassette (ABC) proteins correlates with activation of mitogen activated protein kinase (MAPK) pathway in HCC. Here, we systematically investigated the inhibition of MAPK pathway and its role in regulating HCC cell growth as well as ABC proteins MRP1 and MRP3 expression.

METHODS

The Raf1 kinase inhibitor (GW5074) and different MEK inhibitors (U0126 and AZD6244) were used to treat HCC cells to identify their effects on HCC cell growth and ABC proteins expression in vitro. Cell viability tests were performed after the treatment of MAPK pathway inhibitors and in combination with gemcitabine or doxorubicin. Western blot was applied to assess the changes of MAPK pathway and protein expression of MRP1 and MRP3. Flow cytometry was used to measure intracellular doxorubicin accumulation after the treatment of MEK inhibitors.

RESULTS

Both Raf1 inhibitor (GW5074) and MEK inhibitors (U0126 and AZD6244) suppressed HCC cell growth in a dose dependent manner. Pre-treatment of MEK inhibitor U0126 or AZD6244 sensitized HCC cells to gemcitabine or doxorubicin based chemotherapy. Raf1 inhibitor GW5074 had no effect on MRP1 and MRP3 protein expression. Treatment of gemcitabine or doxorubicin activated phosphorylated ERK and induced the upregulation of MRP1 and MRP3. MEK inhibitors U0126 and AZD6244 deactivated phosphorylated ERK, decreased endogenous MRP1 expression, reversed gemcitabine or doxorubicin induced MRP1 and MRP3 upregulation, and increased the intracellular doxorubicin accumulation.

CONCLUSION

This study provides evidence that MEK inhibitors sensitize HCC cells to chemotherapy by increasing intracellular chemodrug accumulation. MEK inhibirors U0126 and AZD6244 reduced MRP1 as well as MRP3 expression, and may contribute partially to the sensitization. The combination of MEK inhibitor and conventional chemotherapy may offer new therapeutic option for the treatment of resistant HCC.

摘要

背景

肝细胞癌 (HCC) 表现出强烈的内在和获得性药物耐药性，这是化疗的主要障碍。三磷酸腺苷结合盒 (ABC) 蛋白的过度表达与 HCC 中丝裂原活化蛋白激酶 (MAPK) 通路的激活相关。在这里，我们系统地研究了 MAPK 通路的抑制及其在调节 HCC 细胞生长以及 ABC 蛋白 MRP1 和 MRP3 表达中的作用。

方法

使用 Raf1 激酶抑制剂 (GW5074) 和不同的 MEK 抑制剂 (U0126 和 AZD6244) 处理 HCC 细胞，以鉴定它们对 HCC 细胞生长和 ABC 蛋白表达的影响。在用 MAPK 通路抑制剂处理后并与吉西他滨或阿霉素联合用药时进行细胞活力测试。Western blot 用于评估 MAPK 通路和 MRP1 和 MRP3 蛋白表达的变化。流式细胞术用于测量 MEK 抑制剂处理后细胞内阿霉素的积累。

结果

Raf1 抑制剂 (GW5074) 和 MEK 抑制剂 (U0126 和 AZD6244) 均以剂量依赖性方式抑制 HCC 细胞生长。MEK 抑制剂 U0126 或 AZD6244 的预处理使 HCC 细胞对基于吉西他滨或阿霉素的化疗敏感。Raf1 抑制剂 GW5074 对 MRP1 和 MRP3 蛋白表达没有影响。吉西他滨或阿霉素处理激活磷酸化 ERK，并诱导 MRP1 和 MRP3 的上调。MEK 抑制剂 U0126 和 AZD6244 使磷酸化 ERK 失活，降低内源性 MRP1 表达，逆转吉西他滨或阿霉素诱导的 MRP1 和 MRP3 上调，并增加细胞内阿霉素积累。

结论

本研究提供的证据表明，MEK 抑制剂通过增加细胞内化疗药物的积累使 HCC 细胞对化疗敏感。MEK 抑制剂 U0126 和 AZD6244 降低了 MRP1 和 MRP3 的表达，这可能部分有助于增敏。MEK 抑制剂与常规化疗的联合可能为耐药 HCC 的治疗提供新的治疗选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ae49/3558388/001029c6f774/1475-2867-13-3-1.jpg

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MEK 抑制诱导实验性肝细胞癌中 MRP1 和 MRP3 表达下调。

MEK inhibition induced downregulation of MRP1 and MRP3 expression in experimental hepatocellular carcinoma.

机构信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSION

背景

方法

结果

结论

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