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Antiangiogenic and antihepatocellular carcinoma activities of the Juniperus chinensis extract.
Kuo, Zong-Keng; Lin, Mei-Wei; Lu, I-Huang; Yao, Hsin-Jan; Wu, Hsin-Chieh; Wang, Chun-Chung; Lin, Shyh-Horng; Wu, Si-Yuan; Tong, Tien-Soung; Cheng, Yi-Cheng; Yen, Jui-Hung; Ko, Ching-Huai; Chiou, Shu-Jiau; Pan, I-Horng; Tseng, Hsiang-Wen.
Affiliation
  • Kuo ZK; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Lin MW; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Lu IH; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Yao HJ; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Wu HC; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Wang CC; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Lin SH; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Wu SY; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Tong TS; Greenhouse System Technology Center, Industrial Technology Research Institute, Central Region Campus, No.2 Wenxian Rd., Nantou City, 54041, Taiwan.
  • Cheng YC; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Yen JH; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Ko CH; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Chiou SJ; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan.
  • Pan IH; Center of Excellence for Drug Development, Biomedical Technology and Device Research Labs, Industrial Technology Research Institute, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan. I-HorngPan@itri.org.tw.
  • Tseng HW; , Present address: Bldg 13, No. 321, Sec 2, Kuangfu Rd, Hsinchu City, 30011, Taiwan. I-HorngPan@itri.org.tw.
BMC Complement Altern Med ; 16: 277, 2016 Aug 08.
Article in En | MEDLINE | ID: mdl-27502492
ABSTRACT

BACKGROUND:

To identify a novel therapeutic agent for hepatocellular carcinoma (HCC), for which no promising therapeutic agent exists, we screened a panel of plants and found that Juniperus chinensis exhibited potential antiangiogenic and anti-HCC activities. We further investigated the antiangiogenic and anti-HCC effects of the active ingredient of J. chinensis extract, CBT-143-S-F6F7, both in vitro and in vivo.

METHODS:

A tube formation assay conducted using human umbilical vein endothelial cells (HUVECs) was first performed to identify the active ingredient of CBT-143-S-F6F7. A series of angiogenesis studies, including HUVEC migration, Matrigel plug, and chorioallantoic membrane (CAM) assays, were then performed to confirm the effects of CBT-143-S-F6F7 on angiogenesis. The effects of CBT-143-S-F6F7 on tumor growth were investigated using a subcutaneous and orthotopic mouse model of HCC. In vitro studies were performed to investigate the effects of CBT-143-S-F6F7 on the cell cycle and apoptosis in HCC cells. Moreover, protein arrays for angiogenesis and apoptosis were used to discover biomarkers that may be influenced by CBT-143-S-F6F7. Finally, nuclear magnetic resonance analysis was conducted to identify the compounds of CBT-143-S-F6F7.

RESULTS:

CBT-143-S-F6F7 showed significantly antiangiogenic activity in various assays, including HUVEC tube formation and migration, CAM, and Matrigel plug assays. In in vivo studies, gavage with CBT-143-S-F6F7 significantly repressed subcutaneous Huh7 tumor growth in severe combined immunodeficient (SCID) mice, and prolonged the survival of orthotopic Huh7 tumor-bearing SCID mice (a 40 % increase in median survival duration compared with the vehicle-treated mice). Immunohistochemical staining of subcutaneous Huh7 tumors in CBT-143-S-F6F7-treated mice showed a significantly decrease in the cell cycle regulatory protein cyclin D1, cellular proliferation marker Ki-67, and endothelial marker CD31. CBT-143-S-F6F7 caused arrest of the G2/M phase and induced Huh7 cell apoptosis, possibly contributing to the inhibition of HCC tumors. Protein array analysis revealed that several angiogenic and antiapoptotic factors were suppressed in CBT-143-S-F6F7-treated Huh7 cells. Finally, five compounds from CBT-143-S-F6F7 were identified.

CONCLUSIONS:

According to these results, we report for the first time the antiangiogenic and anti-HCC activities of CBT-143-S-F6F7, the active fractional extract of J. chinensis. We believe that CBT-143-S-F6F7 warrants further evaluation as a new anti-HCC drug.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Plant Extracts / Carcinoma, Hepatocellular / Juniperus / Angiogenesis Inhibitors / Liver Neoplasms / Antineoplastic Agents Type of study: Prognostic_studies Limits: Animals / Female / Humans Language: En Journal: BMC Complement Altern Med Journal subject: TERAPIAS COMPLEMENTARES Year: 2016 Document type: Article Affiliation country: Taiwán
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Full text: 1 Collection: 01-internacional Database: MEDLINE Main subject: Plant Extracts / Carcinoma, Hepatocellular / Juniperus / Angiogenesis Inhibitors / Liver Neoplasms / Antineoplastic Agents Type of study: Prognostic_studies Limits: Animals / Female / Humans Language: En Journal: BMC Complement Altern Med Journal subject: TERAPIAS COMPLEMENTARES Year: 2016 Document type: Article Affiliation country: Taiwán