Your search keyword '"Zhang, Yongxing"' showing total 2 results

1. Epac1, PDE4, and PKC protein expression and their association with AKAP95, Cx43, and cyclin D2/ E1 in breast cancer tissues.

Author

Huang, Ping, Sun, Qian, Zhuang, Wenxin, Peng, Kuan, Wang, Dai, Yao, Youliang, Guo, Dongbei, Zhang, Lu, Shen, Chuhan, Sun, Mengyun, Tang, Chaoying, Teng, Bogang, and Zhang, Yongxing

Subjects

BREAST tumors, CELL lines, ESTERASES, GENE expression, IMMUNOHISTOCHEMISTRY, MEMBRANE proteins, TRANSFERASES, CELL cycle proteins

Abstract

Background This study was conducted to investigate the exchange protein directly activated by c AMP ( Epac1), PDE4, and PKC expression in breast cancer tissues, and the correlation between these proteins and AKAP95, Cx43, cyclin D2, and cyclin E1. Methods PV-9000 two-step immunohistochemistry was used to analyze protein expression. Results The positive rate of Epac1 protein expression in breast cancer tissues (58%) was higher than in para-carcinoma tissues (10%) ( P < 0.05). There were no significant differences in the positive rates of PDE4 and PKC expression between breast cancer and para-carcinoma tissues ( P > 0.05). The positive expression rate of PDE4 was higher in the P53 protein positive group compared to the P53 negative group ( P < 0.05). Correlations between Epac1 and cyclin D2, PDE4 and cyclin D2, AKAP95 and PKC, Cx43 and PKC, and cyclin D2 and PKC proteins were observed ( P < 0.05). Conclusion Epac1 expression in breast cancer tissues was increased, suggesting that the protein may be involved in the development of breast cancer. Correlations between Epac1 and cyclin D2, PDE4 and cyclin D2, AKAP95 and PKC, Cx43 and PKC, and cyclin D2 and PKC proteins suggested synergistic effects among these proteins in the development of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2017

2. Epac1, PDE4, and PKC protein expression and their correlation with AKAP95 and Cx43 in esophagus cancer tissues.

Author

Guan, Zhiyu, Zhuang, Winxin, Lei, Hui, Wang, Dai, Yao, Youliang, Guo, Dongbei, Sun, Qian, Chen, Yun, Chen, Xiaoyi, Lin, Hongyan, Teng, Bogang, and Zhang, Yongxing

Subjects

CELL lines, ESOPHAGEAL tumors, ESTERASES, GENE expression, IMMUNOHISTOCHEMISTRY, MEMBRANE proteins, HEALTH outcome assessment, TRANSFERASES, CONNEXINS, CELL cycle proteins

Abstract

Background This study examined the expression of exchange protein directly activated by c AMP1 ( Epac1), PDE4, and PKC in esophageal cancer tissues, and analyzed the association of each protein with the pathological parameters of the samples. Methods Epac1, PDE4, and PKC protein expression was evaluated by PV-9000 two-step immunohistochemical techniques in 51 esophageal cancer specimens and 10 para-carcinoma tissues. Results The positive expression rates of Epac1 and PKC in esophageal cancer tissues (62.7% and 68.6%, respectively) were higher compared to those in para-carcinoma tissues (20% and 20%, respectively) ( P < 0.05). The positive expression rate of PDE4 in esophageal cancer tissues (54.1%) was higher than in para-carcinoma tissues (30%), ( P > 0.05). Epac1, PDE4, and PKC protein expression levels were not associated with the extent of tumor differentiation and/or lymph node metastasis ( P > 0.05). Epac1 protein expression levels correlated with PDE4, PKC, and AKAP95 protein expression levels. In addition, there was a correlation between PKC and Cx43 protein levels ( P < 0.05). Conclusion The expression rates of Epac1, PDE4, and PKC protein in esophageal cancer tissues were significantly higher compared to the rates in para-carcinoma tissues, suggesting an association between these proteins and the development and progression of esophageal cancer. The correlations between these proteins also revealed that they may exert a synergistic effect during the development of esophageal cancer. [ABSTRACT FROM AUTHOR]

Published

2017