Your search keyword '"Zou, Yongxin"' showing total 6 results

1. MicroRNA-26a/b regulate DNA replication licensing, tumorigenesis, and prognosis by targeting CDC6 in lung cancer

Author

Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, He, Jianxing, Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, and He, Jianxing

Abstract

Cancer is characterized by mutations, genome rearrangements, epigenetic changes, and altered gene expression that enhance cell proliferation, invasion, and metastasis. To accommodate deregulated cellular proliferation, many DNA replication-initiation proteins are overexpressed in human cancers. However, the mechanism that represses the expression of these proteins in normal cells and the cellular changes that result in their overexpression are largely unknown. One possible mechanism is through miRNA expression differences. Here, it is demonstrated that miR26a and miR26b inhibit replication licensing and the proliferation, migration, and invasion of lung cancer cells by targeting CDC6. Importantly, miR26a/b expression is significantly decreased in human lung cancer tissue specimens compared with the paired adjacent normal tissues, and miR26a/b downregulation and the consequential upregulation of CDC6 are associated with poorer prognosis of patients with lung cancer. These results indicate that miR26a/b repress replication licensing and tumorigenesis by targeting CDC6.

Published

2014

2. Estrogen receptor α-coupled Bmi1 regulation pathway in breast cancer and its clinical implications

Author

Wang, Huali, Liu, Haijing, Li, Xin, Zhao, Jing, Zhang, Hong, Mao, Jingzhuo, Zou, Yongxin, Zhang, Shuang, Hou, Wei, Hou, Lin, McNutt, Michael A, Zhang, Bo, Wang, Huali, Liu, Haijing, Li, Xin, Zhao, Jing, Zhang, Hong, Mao, Jingzhuo, Zou, Yongxin, Zhang, Shuang, Hou, Wei, Hou, Lin, McNutt, Michael A, and Zhang, Bo

Abstract

Background Bmi1 has been identified as an important regulator in breast cancer, but its relationship with other signaling molecules such as ERα and HER2 is undetermined. Methods The expression of Bmi1 and its correlation with ERα, PR, Ki-67, HER2, p16 INK4a , cyclin D1 and pRB was evaluated by immunohistochemistry in a collection of 92 cases of breast cancer and statistically analyzed. Stimulation of Bmi1 expression by ERα or 17β-estradiol (E2) was analyzed in cell lines including MCF-7, MDA-MB-231, ERα-restored MDA-MB-231 and ERα-knockdown MCF-7 cells. Luciferase reporter and chromatin immunoprecipitation assays were also performed. Results Immunostaining revealed strong correlation of Bmi1 and ERα expression status in breast cancer. Expression of Bmi1 was stimulated by 17β-estradiol in ERα-positive MCF-7 cells but not in ERα-negative MDA-MB-231 cells, while the expression of Bmi1 did not alter expression of ERα. As expected, stimulation of Bmi1 expression could also be achieved in ERα-restored MDA-MB-231 cells, and at the same time depletion of ERα decreased expression of Bmi1. The proximal promoter region of Bmi1 was transcriptionally activated with co-transfection of ERα in luciferase assays, and the interaction of the Bmi1 promoter with ERα was confirmed by chromatin immunoprecipitation. Moreover, in breast cancer tissues activation of the ERα-coupled Bmi1 pathway generally correlated with high levels of cyclin D1, while loss of its activity resulted in aberrant expression of p16 INK4a and a high Ki-67 index, which implied a more aggressive phenotype of breast cancer. Conclusions Expression of Bmi1 is influenced by ERα, and the activity of the ERα-coupled Bmi1 signature impacts p16 INK4a and cyclin D1 status and thus correlates with the tumor molecular subtype and biologic behavior. This demonstrates the important role which is played by ERα-coupled Bmi1 in human breast cancer.

Published

2014

3. MicroRNA-26a/b regulate DNA replication licensing, tumorigenesis, and prognosis by targeting CDC6 in lung cancer

Author

Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, He, Jianxing, Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, and He, Jianxing

Abstract

Cancer is characterized by mutations, genome rearrangements, epigenetic changes, and altered gene expression that enhance cell proliferation, invasion, and metastasis. To accommodate deregulated cellular proliferation, many DNA replication-initiation proteins are overexpressed in human cancers. However, the mechanism that represses the expression of these proteins in normal cells and the cellular changes that result in their overexpression are largely unknown. One possible mechanism is through miRNA expression differences. Here, it is demonstrated that miR26a and miR26b inhibit replication licensing and the proliferation, migration, and invasion of lung cancer cells by targeting CDC6. Importantly, miR26a/b expression is significantly decreased in human lung cancer tissue specimens compared with the paired adjacent normal tissues, and miR26a/b downregulation and the consequential upregulation of CDC6 are associated with poorer prognosis of patients with lung cancer. These results indicate that miR26a/b repress replication licensing and tumorigenesis by targeting CDC6.

Published

2014

4. MicroRNA-26a/b regulate DNA replication licensing, tumorigenesis, and prognosis by targeting CDC6 in lung cancer

Author

Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, He, Jianxing, Zhang, Xin, Xiao, Dakai, Wang, Ziyi, Zou, Yongxin, Huang, Liyan, Lin, Weixuan, Deng, Qiuhua, Pan, Hui, Zhou, Jiangfen, Liang, Chun, and He, Jianxing

Abstract

Cancer is characterized by mutations, genome rearrangements, epigenetic changes, and altered gene expression that enhance cell proliferation, invasion, and metastasis. To accommodate deregulated cellular proliferation, many DNA replication-initiation proteins are overexpressed in human cancers. However, the mechanism that represses the expression of these proteins in normal cells and the cellular changes that result in their overexpression are largely unknown. One possible mechanism is through miRNA expression differences. Here, it is demonstrated that miR26a and miR26b inhibit replication licensing and the proliferation, migration, and invasion of lung cancer cells by targeting CDC6. Importantly, miR26a/b expression is significantly decreased in human lung cancer tissue specimens compared with the paired adjacent normal tissues, and miR26a/b downregulation and the consequential upregulation of CDC6 are associated with poorer prognosis of patients with lung cancer. These results indicate that miR26a/b repress replication licensing and tumorigenesis by targeting CDC6.

Published

2014

5. CUL4B promotes replication licensing by up-regulating the CDK2-CDC6 cascade

Author

Zou, Yongxin, Mi, Jun, Wang, Wenxing, Lu, Juanjuan, Zhao, Wei, Liu, Zhaojian, Hu, Huili, Yang, Yang, Gao, Xiaoxing, Jiang, Baichun, Shao, Changshun, Gong, Yaoqin, Zou, Yongxin, Mi, Jun, Wang, Wenxing, Lu, Juanjuan, Zhao, Wei, Liu, Zhaojian, Hu, Huili, Yang, Yang, Gao, Xiaoxing, Jiang, Baichun, Shao, Changshun, and Gong, Yaoqin

Abstract

Cullin-RING ubiquitin ligases (CRLs) participate in the regulation of diverse cellular processes including cell cycle progression. Mutations in the X-linked CUL4B, a member of the cullin family, cause mental retardation and other developmental abnormalities in humans. Cells that are deficient in CUL4B are severely selected against in vivo in heterozygotes. Here we report a role of CUL4B in the regulation of replication licensing. Strikingly, CDC6, the licensing factor in replication, was positively regulated by CUL4B and contributed to the loading of MCM2 to chromatin. The positive regulation of CDC6 by CUL4B depends on CDK2, which phosphorylates CDC6, protecting it from APC(CDH1)-mediated degradation. Thus, aside being required for cell cycle reentry from quiescence, CDK2 also contributes to pre-replication complex assembly in G1 phase of cycling cells. Interestingly, the up-regulation of CDK2 by CUL4B is achieved via the repression of miR-372 and miR-373, which target CDK2. Our findings thus establish a CUL4B-CDK2-CDC6 cascade in the regulation of DNA replication licensing.

Published

2013

6. CUL4B promotes replication licensing by up-regulating the CDK2-CDC6 cascade

Author

Zou, Yongxin, Mi, Jun, Wang, Wenxing, Lu, Juanjuan, Zhao, Wei, Liu, Zhaojian, Hu, Huili, Yang, Yang, Gao, Xiaoxing, Jiang, Baichun, Shao, Changshun, Gong, Yaoqin, Zou, Yongxin, Mi, Jun, Wang, Wenxing, Lu, Juanjuan, Zhao, Wei, Liu, Zhaojian, Hu, Huili, Yang, Yang, Gao, Xiaoxing, Jiang, Baichun, Shao, Changshun, and Gong, Yaoqin

Abstract

Cullin-RING ubiquitin ligases (CRLs) participate in the regulation of diverse cellular processes including cell cycle progression. Mutations in the X-linked CUL4B, a member of the cullin family, cause mental retardation and other developmental abnormalities in humans. Cells that are deficient in CUL4B are severely selected against in vivo in heterozygotes. Here we report a role of CUL4B in the regulation of replication licensing. Strikingly, CDC6, the licensing factor in replication, was positively regulated by CUL4B and contributed to the loading of MCM2 to chromatin. The positive regulation of CDC6 by CUL4B depends on CDK2, which phosphorylates CDC6, protecting it from APC(CDH1)-mediated degradation. Thus, aside being required for cell cycle reentry from quiescence, CDK2 also contributes to pre-replication complex assembly in G1 phase of cycling cells. Interestingly, the up-regulation of CDK2 by CUL4B is achieved via the repression of miR-372 and miR-373, which target CDK2. Our findings thus establish a CUL4B-CDK2-CDC6 cascade in the regulation of DNA replication licensing.

Published

2013