Formulations combining CpG containing oliogonucleotides and poly I:C enhance the magnitude of immune responses and protection against pancreas disease in Atlantic salmon

被引:34
作者
Strandskog, Guro [1 ]
Villoing, Stephane [2 ]
Iliev, Dimitar B. [1 ]
Thim, Hanna L. [1 ]
Christie, Karen Elina [2 ]
Jorgensen, Jorunn B. [1 ]
机构
[1] Univ Tromso, Norwegian Coll Fisheries Sci, N-9037 Tromso, Norway
[2] Intervet Norbio, N-5008 Bergen, Norway
关键词
Salmon; CpG; Poly I:C; IFN; Innate immunity; Salmon alphavirus; TROUT ONCORHYNCHUS-MYKISS; SINDBIS VIRUS-INFECTION; YELLOW-FEVER VACCINE; SALAR L. LEUKOCYTES; DOUBLE-STRANDED-RNA; REAL-TIME PCR; RAINBOW-TROUT; BACTERIAL-DNA; IN-VITRO; INTERFERON-GAMMA;
D O I
10.1016/j.dci.2011.03.016
中图分类号
S9 [水产、渔业];
学科分类号
0908 ;
摘要
Both CpG oligodeoxynucleotides and double-stranded RNA (poly I:C) have documented effects as treatments against several viral diseases in fish. However, as stand-alone treatments their effects have been modest. We have tested here whether CpG and poly I:C, alone or in combination induce protection against Salmonid Alphavirus (SAV), the causative agent of pancreas disease in Atlantic salmon. Our results revealed a significant reduction of viraemia 2 weeks after ip injection of the combined treatment and 1 week after challenge with SAV subtype 3, followed by reduced SAV induced heart pathology 3 weeks later. The SAV titers in blood samples from the combination group were lower as compared to single treatments with either CpG or poly I:C. Surprisingly, reduced SAV levels could also be found in fish as long as 7 weeks after receiving the combination treatment. The expression of IFN gamma and to a lesser extent IFNa and Mx was up-regulated in head kidney and spleen 5 days after the fish had been treated with CpG and poly I:C. Furthermore, the complement factor C4 was depleted in serum 8 weeks post treatment, suggesting complement activation leading to C4 consumption. We hypothesize that the CpG/poly I:C-induced protection against SAV3 is mediated by mechanisms involving type I and type II IFN induced antiviral activity and complement mediated protective responses. (C) 2011 Elsevier Ltd. All rights reserved.
引用
收藏
页码:1116 / 1127
页数:12
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