Diwan Manish, Tafaghodi Mohsen, Samuel John
Faculty of Pharmacy and Pharmaceutical Sciences, 3118 Dentistry/Pharmacy Center, University of Alberta, Edmonton, T6G 2N8 Canada.
J Control Release. 2002 Dec 13;85(1-3):247-62. doi: 10.1016/s0168-3659(02)00275-4.
Synthetic oligodeoxynucleotides (ODN) consisting of unmethylated bacterial DNA sequences with CpG motifs are potent immunological adjuvants. Immunostimulatory CpG sequences are species-specific. Optimal CpG sequences specific for humans, rodents, livestock, and companion animals have been reported. Nearly all of these reports describe the use of soluble forms of CpG ODN and antigens. We investigated the co-delivery of CpG ODN and antigens in biodegradable nanospheres as an alternative approach for immunization using tetanus toxoid (TT) as the model antigen and ODN #1826 as the model CpG sequence. TT and CpG ODN were co-encapsulated in poly(D,L-lactic-co-glycolic acid) nanospheres. Separate groups of C57BL/6 mice were subcutaneously immunized twice with TT and CpG ODN in nanospheres (test group), TT alone in nanospheres, TT alone in nanospheres mixed with CpG ODN in solution, TT and CpG ODN both in solution (reference group), TT alone in solution, and alum adsorbed TT. T cells isolated from the test group showed strong antigen-specific T cell proliferation ex vivo (stimulation index=45). This was significantly (P<0.0001) higher than that observed for T cells isolated from the reference group. The T cell proliferation of the test group was associated with higher levels of interferon gamma secretion (IFN-gamma 2694.7+/-41.1 pg/ml) than that of the reference group (814.7+/-50.2 pg/ml). Interleukin 4 (IL-4) secretion, if any, was below the detection limit (<13 pg/ml) in all the groups. Anti-sera obtained from the test group also showed very high total IgG titers (end point titers, 2560000) that were 16 times higher than the reference group. Similarly, differences of 8-fold for IgG1 and IgG3, and 5-fold for IgG2b titers were observed. Noticeably, the antibody response induced in the alum-TT group was far less (total IgG, end point titers 160000) than that obtained in the TT-CpG ODN nanospheres group. Overall, the results show that co-delivery of CpG and TT resulted in induction of both T helper type 1 and type 2 (Th1 and Th2) immune responses with a bias towards Th1 type. These results suggest that the co-delivery of CpG ODN adjuvants and antigens in nanospheres is a more efficient approach for immunization than the use of CpG ODN and TT in solution.
由含有CpG基序的未甲基化细菌DNA序列组成的合成寡脱氧核苷酸(ODN)是强效免疫佐剂。免疫刺激性CpG序列具有物种特异性。已经报道了对人类、啮齿动物、家畜和伴侣动物具有特异性的最佳CpG序列。几乎所有这些报道都描述了使用可溶性形式的CpG ODN和抗原。我们研究了在可生物降解纳米球中共递送CpG ODN和抗原,作为一种替代的免疫方法,使用破伤风类毒素(TT)作为模型抗原,ODN #1826作为模型CpG序列。TT和CpG ODN被共包封在聚(D,L-乳酸-共-乙醇酸)纳米球中。将单独的C57BL/6小鼠组皮下免疫两次,分别用纳米球中的TT和CpG ODN(试验组)、单独纳米球中的TT、单独纳米球中的TT与溶液中的CpG ODN混合、溶液中的TT和CpG ODN(参考组)、单独溶液中的TT以及明矾吸附的TT。从试验组分离的T细胞在体外显示出强烈的抗原特异性T细胞增殖(刺激指数 = 45)。这显著(P<0.0001)高于从参考组分离的T细胞所观察到的值。试验组的T细胞增殖与比参考组更高水平的干扰素γ分泌(IFN-γ 2694.7±41.1 pg/ml)相关。所有组中白细胞介素4(IL-4)分泌(如果有的话)低于检测限(<13 pg/ml)。从试验组获得的抗血清也显示出非常高的总IgG滴度(终点滴度,2560000),比参考组高16倍。同样,观察到IgG1和IgG3滴度有8倍差异,IgG2b滴度有5倍差异。值得注意的是,明矾-TT组诱导的抗体反应远低于(总IgG,终点滴度160000)TT-CpG ODN纳米球组获得的反应。总体而言,结果表明CpG和TT的共递送导致诱导1型和2型辅助性T细胞(Th1和Th2)免疫反应,且偏向Th1型。这些结果表明在纳米球中共递送CpG ODN佐剂和抗原是一种比在溶液中使用CpG ODN和TT更有效的免疫方法。
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