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Chicken HSP70 DNA vaccine inhibits tumor growth in a canine cancer model
Authors:Yu Wen-Ying  Chuang Tien-Fu  Guichard Cécile  El-Garch Hanane  Tierny Dominique  Laio Albert Taiching  Lin Ching-Si  Chiou Kuo-Hao  Tsai Cheng-Long  Liu Chen-Hsuan  Li Wen-Chiuan  Fischer Laurent  Chu Rea-Min
Affiliation:a Animal Cancer Center, School of Veterinary Medicine, National Taiwan University, Taipei, Taiwan, ROC
b Merial S.A.S., R&D, Laboratoire de Lyon Gerland, 254 rue Marcel Mérieux, 69007 Lyon, France
c Oncovet, Villeneuve d’Ascq, France
d School of Veterinary Medicine, National Taiwan University, Taipei, Taiwan, ROC
e Animal Technology of Institute, Maoli, Taiwan, ROC
Abstract:
Immunization with xenogeneic DNA is a promising cancer treatment to overcome tolerance to self-antigens. Heat shock protein 70 (HSP70) is over-expressed in various kinds of tumors and is believed to be involved in tumor progression. This study tested a xenogeneic chicken HSP70 (chHSP70) DNA vaccine in an experimental canine transmissible venereal tumor (CTVT) model. Three vaccination strategies were compared: the first (PE) was designed to evaluate the prophylactic efficacy of chHSP70 DNA vaccination by delivering the vaccine before tumor inoculation in a prime boost setting, the second (T) was designed to evaluate the therapeutic efficacy of the same prime boost vaccine by vaccinating the dogs after tumor inoculation; the third (PT) was similar to the first strategy (PE), with the exception that the electroporation booster injection was replaced with a transdermal needle-free injection. Tumor growth was notably inhibited only in the PE dogs, in which the vaccination program triggered tumor regression significantly sooner than in control dogs (NT). The CD4+ subpopulation of tumor-infiltrating lymphocytes and canine HSP70 (caHSP70)-specific IFN-γ-secreting lymphocytes were significantly increased during tumor regression in the PE dogs as compared to control dogs, demonstrating that specific tolerance to caHSP70 has been overcome. In contrast, no benefit of the therapeutic strategy (T) could be noticed and the (PT) strategy only led to partial control of tumor growth. In summary, antitumor prophylactic activity was demonstrated using the chHSP70 DNA vaccine including a boost via electroporation. Our data stressed the importance of DNA electroporation as a booster to get the full benefit of DNA vaccination but also of cancer immunotherapy initiation as early as possible. Xenogeneic chHSP70 DNA vaccination including an electroporation boost is a potential vaccine to HSP70-expressing tumors, although further research is still required to better understand true clinical potential.
Keywords:Xenogeneic DNA vaccine   HSP70   Electroporation   Transdermal injection   CTVT
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