- 作者:Chun Yeha ; Chun-Chia Chengb ; cccheng@iner.gov.tw" class="auth_mail" title="E-mail the corresponding author ; Hua-Ching Linc ; Tsai-Yueh Luob ; Jungshan Changd ; Ai-Sheng Hoa ; aisheng49@gmail.com" class="auth_mail" title="E-mail the corresponding author
- 关键词:Apolipoprotein A1 ; Colorectal cancer ; Gastric cancer ; Pravastatin
- 刊名:Advances in Digestive Medicine
- 出版年:2016
- 出版时间:March 2016
- 年:2016
- 卷:3
- 期:1
- 页码:3-10
- 全文大小:1103 K
Methods
Pravastatin-induced inhibition in tumor proliferation in vitro and in xenografts was investigated. Reduced ApoA1 expressions were detected in the tumor regions in specimens from tumor patients as well in xenografts using Western Blotting. Moreover, ApoA1 was administered to inhibit tumor proliferation, and pravastatin was given to enhance the chemotherapeutic efficacy of doxorubicin (DOX).
Results
We found a significant statistical reduction of ApoA1 in the tumor regions of specimens from gastric cancer and colorectal cancer patients. MKN45 cells proliferation was inhibited by 18% under the growing medium containing pravastatin. ApoA1 levels were elevated in liver Clone 9 cells administered pravastatin, but not in MKN45 cells. In vitro studies revealed that ApoA1 can reduce MKN45 tumor proliferation. Moreover, the tumor volume was significantly reduced in in vivo xenografts after the administration of pravastatin. Combined treatments of pravastatin with DOX significantly minimized the size of tumors, leading to a better therapeutic efficacy.
Conclusion
This study demonstrated that pravastatin elevated ApoA1, an HDL major constituent with anti-inflammatory characteristics, which displayed strong adversary associations with tumor developments and growth. Increasing the amounts of ApoA1 by pravastatin coupled with DOX may improve the therapeutic efficacy for cancer treatment.