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A DNA-priming protein-boosting regimen significantly improves type 1 immune response but not protective immunity to Trypanosoma cruzi infection in a highly susceptible mouse strain

机译：DNA引发蛋白的增强方案可显着改善1型免疫应答，但不能改善对高度易感小鼠品系中克氏锥虫感染的保护性免疫

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BALB/c or C57Bl/6 mice immunized with plasmids containing Trypanosoma cruzi genes developed specific immune responses and protective immunity against lethal parasitic infection. in contrast, in the highly susceptible mouse strain A/Sn, DNA vaccination reduced the peak parasitemia but promoted limited mouse survival after challenge. in the present study, we tested whether the immunogenicity and protective efficacy of vaccination could be improved by combining DNA and recombinant protein immunization regimens. A/Sn mice immunized with plasmid p154/13 which harbours the gene encoding Trypanosoma cruzi trans -sialidase developed a predominant type 1 immune response. in contrast, immunization with the recombinant Trypanosoma cruzi trans -sialidase protein adsorbed to alum generated a typical type 2 immune response. Simultaneous administration of both p154/13 and recombinant Trypanosoma cruzi trans -sialidase protein also led to a predominant type 2 immune response. Sequential immunization consisting of two priming doses of p154/13 followed by booster injections with recombinant Trypanosoma cruzi trans -sialidase protein significantly improved specific type 1 immune response, as revealed by a drastic reduction of the serum IgG1/IgG2a ratio and by an increase in the in vitro interferon-gamma secretion by CD4 T cells. Our observations confirm and extend previous data showing that a DNA-priming protein-boosting regimen might be a general strategy to enhance type 1 immune response to DNA vaccines. Upon challenge with Trypanosoma cruzi , no improvement in protective immunity was observed in mice immunized with the DNA-priming protein-boosting regimen when compared to animals that received DNA only. Therefore, our results suggest that in this experimental model there is no correlation between the magnitude of type 1 immune response and protective immunity against Trypanosoma cruzi infection.

机译：用含有克鲁斯锥虫基因的质粒免疫的BALB / c或C57Bl / 6小鼠表现出特异性免疫应答和针对致命性寄生虫感染的保护性免疫。相反，在高度易感的小鼠品系A / Sn中，DNA疫苗接种减少了峰值寄生虫血症，但促进了攻击后小鼠的有限存活。在本研究中，我们测试了通过结合DNA和重组蛋白免疫方案能否提高疫苗的免疫原性和保护效力。用具有编码克鲁斯锥虫反唾液酸酶基因的质粒p154 / 13免疫的A / Sn小鼠产生了主要的1型免疫应答。相反，用吸附到明矾上的重组克鲁斯锥虫反唾液酸酶蛋白免疫可产生典型的2型免疫应答。同时施用p154 / 13和重组克鲁斯锥虫反唾液酸酶蛋白也导致了主要的2型免疫反应。序贯免疫包括两次初次接种的p154 / 13剂量，然后再次注射重组克鲁氏锥虫反唾液酸酶蛋白，显着改善了特异性1型免疫反应，这可以通过血清IgG1 / IgG2a比例的急剧降低和血清中IgG1 / IgG2a比例的增加来揭示。 CD4 T细胞的体外γ干扰素分泌。我们的观察结果证实并扩展了以前的数据，这些数据表明DNA引发蛋白增强方案可能是增强对DNA疫苗的1型免疫应答的一般策略。用克氏锥虫攻击后，与仅接受DNA的动物相比，在使用DNA引发蛋白增强方案免疫的小鼠中未观察到保护性免疫的改善。因此，我们的结果表明，在该实验模型中，1型免疫反应的强度与克氏锥虫感染的保护性免疫之间没有相关性。

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Vasconcelos Jose Ronnie Carvalho de; Boscardin Silvia Beatriz; Hiyane Meire Ioshie; Kinoshita Sheila Sayumi; Fujimura Adriana Erika; Rodrigues Mauricio Martins;
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1. A DNA-priming protein-boosting regimen significantly improves type 1 immune response but not protective immunity to Trypanosoma cruzi infection in a highly susceptible mouse strain. [J] . Vasconcelos JR, Boscardin SB, Hiyane MI, Immunology and Cell Biology . 2003,第2期

机译：在高易感小鼠品系中，DNA引发蛋白增强方案可显着改善1型免疫应答，但不能改善对克鲁斯锥虫感染的保护性免疫。
2. Redirection of the immune response to the functional catalytic domain of the cystein proteinase cruzipain improves protective immunity against Trypanosoma cruzi infection. [J] . Cazorla SI, Frank FM, Becker PD, The Journal of Infectious Diseases . 2010,第1期

机译：将免疫应答重定向至半胱氨酸蛋白酶克鲁兹痛的功能性催化结构域可改善针对克鲁斯锥虫感染的保护性免疫力。
3. Redirection of the Immune Response to the Functional Catalytic Domain of the Cystein Proteinase Cruzipain Improves Protective Immunity against Trypanosoma cruzi Infection [J] . Silvia I. Cazorla, Fernanda M. Frank, Pablo D. Becker, Journal of Infectious Diseases . 2010,第1期

机译：对半胱氨酸蛋白酶克鲁兹疼痛的功能性催化域的免疫反应的重定向提高了针对克鲁氏锥虫感染的保护性免疫。
4. Different peripheral neuroendocrine responses to Trypanosoma cruzi infection in mice lacking adaptive immunity [C] . Eduardo Roggero, Johannes Wildmann, Marcelo O. Passerini, International Society for Neuroimmunomodulation . 2012

机译：不同周围神经内分泌反应对缺乏适应性免疫的小鼠脑蛋白酶瘤Cruzi感染
5. Effects of fumonisins on selected murine immune responses and infection with Trypanosoma cruzi (Fusarium moniliforme). [D] . Dresden-Osborne, Charissa Deanne. 2001

机译：伏马菌素对选择的鼠类免疫反应和克氏锥虫的感染的影响。
6. Novel Protective Antigens Expressed by Trypanosoma cruzi Amastigotes Provide Immunity to Mice Highly Susceptible to Chagas Disease [O] . Eduardo L. V. Silveira, Carla Claser, Filipe A. B. Haolla, 2008

机译：克氏锥虫Amastigotes表达的新型保护性抗原可为高度易患南美锥虫病的小鼠提供免疫力
7. Redirection of the immune response to the functional catalytic domain of the cystein proteinase cruzipain improves protective immunity against Trypanosoma cruzi infection. [O] . Cazorla, Silvia I, Frank, Fernanda M, Becker, Pablo D, 2010

机译：将免疫应答重定向至半胱氨酸蛋白酶克鲁兹痛的功能性催化结构域可改善针对克鲁斯锥虫感染的保护性免疫力。
8. The Cellular and Humoral Immune Response to 'Schistosoma mansoni' Infections in Inbred Rats. III. Development of Optimal Protective Immunity Following Natural Infections and Artificial Immunizations. [R] . Phillips, S. M., Reid, W. A., Doughty, B., 1977

机译：近交系大鼠'曼氏血吸虫'感染的细胞和体液免疫应答。 III。自然感染和人工免疫后最佳保护性免疫的研究进展。

A DNA-priming protein-boosting regimen significantly improves type 1 immune response but not protective immunity to Trypanosoma cruzi infection in a highly susceptible mouse strain

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