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KMID : 0620920090410110812
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Experimental & Molecular Medicine
2009 Volume.41 No. 11 p.812 ~ p.823
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Modulation of protective immunity against herpes simplex virus via mucosal genetic co-transfer of DNA vaccine with ¥â2-adrenergic agonist
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Kim Seong-Bum
Han Young-Woo
Rahman M.M.
Kim Seon-Ju
Yoo Dong-Jin
Kang Seong-Ho
Kim Koan-Hoi
Eo Seong-Kug
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Abstract
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Cholera toxin, which has been frequently used as mucosal adjuvant, leads to an irreversible activation of adenylyl cyclase, thereby accumulating cAMP in target cells. Here, it was assumed that ¥â2-adrenergic agonist salbutamol may have modulatory functions of immunity induced by DNA vaccine, since ¥â2-adrenergic agonists induce a temporary cAMP accumulation. To test this assumption, the present study evaluated the modulatory functions of salbutamol co-administered with DNA vaccine expressing gB of herpes simplex virus (HSV) via intranasal (i.n.) route. We found that the i.n. co-administration of salbutamol enhanced gB-specific IgG and IgA responses in both systemic and mucosal tissues, but optimal dosages of co-administered salbutamol were required to induce maximal immune responses. Moreover, the mucosal co-delivery of salbutamol with HSV DNA vaccine induced Th2-biased immunity against HSV antigen, as evidenced by IgG isotypes and Th1/Th2-type cytokine production. The enhanced immune responses caused by co-administration of salbutamol provided effective and rapid responses to HSV mucosal challenge, thereby conferring prolonged survival and reduced inflammation against viral infection. Therefore, these results suggest that salbutamol may be an attractive adjuvant for mucosal genetic transfer of DNA vaccine.
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KEYWORD
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albuterol, herpes simplex virus vaccines, immunity, mucosal, Th1 cells, Th2 cells, vaccine, DNA
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