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Chinese Archives of General Surgery(Electronic Edition) ›› 2013, Vol. 07 ›› Issue (04): 298-302. doi: 10.3877/cma.j.issn.1674-0793.2013.04.013

Special Issue:

• Original Article • Previous Articles     Next Articles

Experimental study of β-GC combined with HBsAg gene-modified dendritic cell-based tumor vaccine to hepatocellular carcinoma by different immune ways

Qiang-sheng DAI1, He-ping LI2,(), Jian-ting LONG1, Rui-fang ZENG1, Bing ZHANG2, Bo ZHOU2, Si-zhong XING3, Zhi-rong ZENG4, Wei CHEN2, Jian-yong YANG2   

  1. 1. Department of Oncology, the First Affiliated Hospital of Sun Yat-sen University, Guangzhou 510080 , China
  • Received:2013-04-27 Online:2013-08-01 Published:2013-08-01
  • Contact: He-ping LI
  • About author:
    Corresponding author: LI He-ping, Email:

Abstract:

Objective

To explore the efficacy of β-GC combined with HBsAg gene-modified DC vaccine on animal model with HCC using different immunization routes.

Methods

Recombinant adenovirus vector-mediated HBsAg gene-modified DC was used to construct HBsAg-DC which was infused into C57BL/6J mice bearing HBsAg-related HCC by subcutaneous injection. Mice in group A, B and C were vaccinated with PBS, group D, E and F were vaccinated with pAd-HBsAg-DC twice before HepG2 22.1.5 inoculation as described above. Starting at the day of inoculation, mice were treated with daily intra-peritoneal. (ip, 1.5μg per mouse) β-GC injection in group B and E or daily oral β-GC doses(po, 15μg per mouse) in group C and F. Group A and D receiving vehicle (po) were set as control for β-GC treatment.The effectiveness of the immune therapy on tumor growth was compared among different groups.

Results

Tumor size measured 36 days after inoculation was (364.2±3.06)mm3 in group A, (236.5±8.96)mm3 in group B, (251.0±5.76)mm3 in group C, (75.0±5.9)mm3 in group D, (35.3±4.46)mm3 in group E, and (38.5±5.47)mm3 in group F. The application of β-GC demonstrated anti-tumor activity by itself (group B and C), and also enhanced the tumor preventive effect of pAd-HBsAg-DC (group E and F). No difference in tumor growth was observed between ip and po application of β-GC.

Conclusion

β-GC may serve as an immune enhancer to augment the anti-tumor immunity triggered by HBsAg gene-modified DC vaccine. It's antitumor effect may be related to activation of NKT cells.

Key words: Dendritic cells (DC), HBs-Ag gene, HepG2 22.1.5 hepatoma cells, Vaccine, Gene therapy, β-GC

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