MAPK11/12/13/14（p38丝裂原活化蛋白激酶）信号通路的激活可调节自噬基因的转录，以响应新型铜复合物在HeLa细胞中诱导产生的氧化应激。

Activation of the MAPK11/12/13/14 (p38 MAPK) pathway regulates the transcription of autophagy genes in response to oxidative stress induced by a novel copper complex in HeLa cells.

作者信息

Zhong Wu, Zhu Haichuan, Sheng Fugeng, Tian Yonglu, Zhou Jun, Chen Yingyu, Li Song, Lin Jian

机构信息

Laboratory of Computer-Aided Drug Design and Discovery; Beijing Institute of Pharmacology and Toxicology; Beijing, China.

Laboratory of Computer-Aided Drug Design and Discovery; Beijing Institute of Pharmacology and Toxicology; Beijing, China; Synthetic and Functional Biomolecules Center; College of Chemistry and Molecular Engineering; Peking University; Beijing, China.

出版信息

Autophagy. 2014 Jul;10(7):1285-300. doi: 10.4161/auto.28789. Epub 2014 May 13.

DOI:10.4161/auto.28789

PMID:24905917

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4203553/

Abstract

Transition metal copper (Cu) can exist in oxidized or reduced states in cells, leading to cytotoxicity in cancer cells through oxidative stress. Recently, copper complexes are emerging as a new class of anticancer compounds. Here, we report that a novel anticancer copper complex (HYF127c/Cu) induces oxidative stress-dependent cell death in cancer cells. Further, transcriptional analysis revealed that oxidative stress elicits broad transcriptional changes of genes, in which autophagy-related genes are significantly changed in HYF127c/Cu-treated cells. Consistently, autophagy was induced in HYF127c/Cu-treated cells and inhibitors of autophagy promoted cell death induced by HYF127c/Cu. Further analysis identified that the MAPK11/12/13/14 (formerly known as p38 MAPK) pathway was also activated in HYF127c/Cu-treated cells. Meanwhile, the MAPK11/12/13/14 inhibitor SB203580 downregulated autophagy by inhibiting the transcription of the autophagy genes MAP1LC3B, BAG3, and HSPA1A, and promoted HYF127c/Cu-induced cell death. These data suggest that copper-induced oxidative stress will induce protective autophagy through transcriptional regulation of autophagy genes by activation of the MAPK11/12/13/14 pathway in HeLa cells.

摘要

过渡金属铜（Cu）在细胞中可以以氧化态或还原态存在，通过氧化应激导致癌细胞产生细胞毒性。最近，铜配合物正作为一类新型抗癌化合物出现。在此，我们报告一种新型抗癌铜配合物（HYF127c/Cu）在癌细胞中诱导氧化应激依赖性细胞死亡。此外，转录分析显示氧化应激引发基因的广泛转录变化，其中自噬相关基因在经HYF127c/Cu处理的细胞中显著改变。一致地，在经HYF127c/Cu处理的细胞中诱导了自噬，并且自噬抑制剂促进了HYF127c/Cu诱导的细胞死亡。进一步分析确定，在经HYF127c/Cu处理的细胞中MAPK11/12/13/14（以前称为p38 MAPK）途径也被激活。同时，MAPK11/12/13/14抑制剂SB203580通过抑制自噬基因MAP1LC3B、BAG3和HSPA1A的转录下调自噬，并促进HYF127c/Cu诱导的细胞死亡。这些数据表明，铜诱导的氧化应激将通过激活HeLa细胞中的MAPK11/12/13/14途径对自噬基因进行转录调控来诱导保护性自噬。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/42df/4203553/aaa529b954f9/auto-10-1285-g1.jpg

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MAPK11/12/13/14（p38丝裂原活化蛋白激酶）信号通路的激活可调节自噬基因的转录，以响应新型铜复合物在HeLa细胞中诱导产生的氧化应激。

Activation of the MAPK11/12/13/14 (p38 MAPK) pathway regulates the transcription of autophagy genes in response to oxidative stress induced by a novel copper complex in HeLa cells.

作者信息

Zhong Wu, Zhu Haichuan, Sheng Fugeng, Tian Yonglu, Zhou Jun, Chen Yingyu, Li Song, Lin Jian

机构信息

Laboratory of Computer-Aided Drug Design and Discovery; Beijing Institute of Pharmacology and Toxicology; Beijing, China.

出版信息

Autophagy. 2014 Jul;10(7):1285-300. doi: 10.4161/auto.28789. Epub 2014 May 13.

DOI:10.4161/auto.28789

PMID:24905917

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4203553/

Abstract

摘要

MAPK11/12/13/14（p38丝裂原活化蛋白激酶）信号通路的激活可调节自噬基因的转录，以响应新型铜复合物在HeLa细胞中诱导产生的氧化应激。

Activation of the MAPK11/12/13/14 (p38 MAPK) pathway regulates the transcription of autophagy genes in response to oxidative stress induced by a novel copper complex in HeLa cells.

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MAPK11/12/13/14（p38丝裂原活化蛋白激酶）信号通路的激活可调节自噬基因的转录，以响应新型铜复合物在HeLa细胞中诱导产生的氧化应激。

Activation of the MAPK11/12/13/14 (p38 MAPK) pathway regulates the transcription of autophagy genes in response to oxidative stress induced by a novel copper complex in HeLa cells.

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