Adjuvant activities of immune response modifier R-848: Comparison with CpG ODN

被引:128
作者
Vasilakos, JP [1 ]
Smith, RMA
Gibson, SJ
Lindh, JM
Pederson, LK
Reiter, MJ
Smith, MH
Tomai, NA
机构
[1] 3M Co, Pharmaceut, Dept Pharmacol, 3M Ctr, St Paul, MN 55144 USA
[2] 3M Co, Pharmaceut, Dept Med Operat Biostat, 3M Ctr, St Paul, MN 55144 USA
关键词
immunomodulators; vaccination; cytokines; isotype switching; Th1/Th2;
D O I
10.1006/cimm.2000.1689
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
R-848 and imiquimod belong to a class of immune response modifiers that are potent inducers of cytokines, including IFN-alpha; TNF-alpha, IL-12, and lFN-gamma. Many of these cytokines can affect the acquired immune response. This study examines the effects of R-848 on aspects of acquired immunity, including immunoglobulin secretion, in vivo cytokine production, and Ag-specific T cell cytokine production. Results are compared with those of Th1 CpG ODN. R-848 and CpG; ODN are effective at skewing immunity in the presence of Alum toward a Th1 Ab response (IgG2a) and away from a Th2 Ab response (IgE). R-848 and CpG ODN are also capable of initiating an immune response in the absence of additional adjuvant by specifically enhancing IgG2a levels. Both R-848 and imiquimod showed activity when given subcutaneously or orally, indicating that the compound mechanism was not through generation of a depot effect. Although CpG ODN behaves similarly to R-848, CpG; ODN has a distinct cytokine profile, is more effective than R-848 when given with Alum in the priming dose, and is active only when given by the same route as the Ag. The mechanism of R-848's adjuvant activity is linked to cytokine production, where increases in IgG2a levels are associated with IFN-alpha, TNF-alpha; IL-12, and IFN-gamma induction, and decreases in IgE levels are associated with IFN-alpha and TNF-alpha. Imiquimod also enhances IgG2a production when given with Ag. The above results suggest that the imidazoquinolines R-848 and imiquimod may be attractive compounds for use as vaccine adjuvants and in inhibiting pathological responses mediated by Th2 cytokines. (C) 2000 Academic Press.
引用
收藏
页码:64 / 74
页数:11
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