首页> 美国卫生研究院文献>Experimental and Therapeutic Medicine >Intramuscular primary immunization by nucleic acid vaccine pcDNA/Gpd-IL-2 and enhanced immunization with mucosal adjuvant CpG-ODN and Gpd-IL-2 recombinant protein effectively induced strong mucosal immune responses and immune protective effects against Treponema pallidum skin infection
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Intramuscular primary immunization by nucleic acid vaccine pcDNA/Gpd-IL-2 and enhanced immunization with mucosal adjuvant CpG-ODN and Gpd-IL-2 recombinant protein effectively induced strong mucosal immune responses and immune protective effects against Treponema pallidum skin infection

机译:核酸疫苗pcDNA / Gpd-IL-2的肌内一次免疫以及粘膜佐剂CpG-ODN和Gpd-IL-2重组蛋白的增强免疫有效诱导了强烈的粘膜免疫反应和针对梅毒螺旋体皮肤感染的免疫保护作用

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摘要

The present study aimed to evaluate the immune effect of intramuscular primary immunization by the nucleic acid vaccine pcDNA/glycerophosphodiester phosphodiesterase-interleukin-2 (pcDNA/Gpd-IL-2) and enhanced immunization 2 weeks later with the combination of mucosal adjuvant CpG-oligodeoxynucleotides (ODN) and Gpd-IL-2 recombinant protein on skin infection caused by Treponema pallidum (Tp) in New Zealand rabbits. At week 8 following immunization, MTT assay was used to detect spleen cell proliferation, while enzyme-linked immunosorbent assay was performed to detect the cytokine and secretory immunoglobulin A (SIgA) levels. At week 10 after primary immunization, rabbits were inoculated with 105 Tp (Nichols strain). Alterations in the skin redness, swelling and ulceration were recorded for 0–60 days. In addition, positive rate of Tp in skin lesions and ulcer formation rate were examined using dark field and silver staining. The results indicated that intramuscular primary immunization by nucleic acid vaccine pcDNA/Gpd-IL-2 followed by enhanced immunization via nasal feeding with mucosal adjuvant CpG-ODN and Gpd-IL-2 recombinant protein induced the higher levels of Tp Gpd specific antibodies, increased the secretion of IL-2 and interferon-γ, and promoted the proliferation of T cells in the first 8 weeks after immunization. Furthermore, this immunization strategy stimulated the production of mucosa specific SIgA antibody. Thus, this strategy led to the lowest Tp positive and ulcer formation rates at the Tp infection sites, as well as healing of skin lesions on the earliest time point (day 42). In conclusion, immunization by nucleic acid vaccine pcDNA/Gpd-IL-2 followed by enhanced immunization with a combination of mucosal adjuvant CpG-ODN and Gpd-IL-2 recombinant protein is an effective immune strategy to induce strong mucosal immune responses and immune protective effects.
机译:本研究旨在评估核酸疫苗pcDNA /甘油磷酸二酯磷酸二酯酶-白介素2(pcDNA / Gpd-IL-2)进行的肌肉一次免疫的免疫效果,并在2周后与粘膜佐剂CpG-寡脱氧核苷酸联合使用来增强免疫效果。 (ODN)和Gpd-IL-2重组蛋白对新西兰兔中梅毒螺旋体(Tp)引起的皮肤感染的作用。免疫后第8周,MTT分析用于检测脾细胞增殖,而酶联免疫吸附分析用于检测细胞因子和分泌性免疫球蛋白A(SIgA)水平。初次免疫后第10周,给兔子接种10 5 Tp(尼科尔斯毒株)。记录了0至60天的皮肤发红,肿胀和溃疡的变化。此外,使用暗视野和银染检查了皮肤病变中Tp的阳性率和溃疡形成率。结果表明,通过核酸疫苗pcDNA / Gpd-IL-2进行的肌肉内一次免疫,然后通过鼻饲粘膜佐剂CpG-ODN和Gpd-IL-2重组蛋白进行的增强免疫诱导了更高水平的Tp Gpd特异性抗体升高。免疫后头8周IL-2和干扰素-γ的分泌,促进T细胞的增殖。此外,这种免疫策略刺激了粘膜特异性SIgA抗体的产生。因此,该策略导致Tp感染部位的Tp阳性和溃疡形成率最低,并且最早时间点(第42天)皮肤损伤的愈合。总之,通过核酸疫苗pcDNA / Gpd-IL-2进行免疫,然后结合粘膜佐剂CpG-ODN和Gpd-IL-2重组蛋白进行增强免疫,是诱导强烈的粘膜免疫应答和免疫保护作用的有效免疫策略。效果。

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