Enhanced immunoprotective potential of Mycobacterium tuberculosis Ag85 complex protein based vaccine against airway Mycobacterium tuberculosis challenge following intranasal administration.

Giri PK; Verma I; Khuller GK

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Enhanced immunoprotective potential of Mycobacterium tuberculosis Ag85 complex protein based vaccine against airway Mycobacterium tuberculosis challenge following intranasal administration.

机译：鼻内给药后，结核分枝杆菌基于Ag85复合蛋白的疫苗针对气道结核分枝杆菌攻击的疫苗具有增强的免疫保护潜力。

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This study examined the role of intranasal vaccination with Mycobacterium tuberculosis antigen85 complex proteins formulated in dimethyldioctadecylammonium bromide against airway Mycobacterium tuberculosis challenge in mice. Intranasal vaccination with antigen85A and antigen85B induced a significantly higher level of interferon-gamma, interleukin-12 and interleukin-4 in cervical lymph nodes together with IgA and IgG, predominantly IgG2a isotype in nasal secretion over subcutaneous vaccination. Further, intranasal vaccination with antigen85A and antigen85B imparted protection comparable with that obtained from intranasal or subcutaneous Mycobacterium bovis bacillus Calmette-Guerin immunization. These results suggest that mucosal vaccination via the intranasal route is of importance in the development of vaccine for tuberculosis.

机译：这项研究检查了鼻内接种结核分枝杆菌抗原85复合蛋白配制的溴化二甲基二十八烷基氨化铵对小鼠气道结核分枝杆菌攻击的作用。经鼻内接种抗原85A和抗原85B可以在宫颈淋巴结中诱导更高水平的干扰素-γ，白细胞介素12和白细胞介素-4以及IgA和IgG，主要是皮下疫苗经鼻分泌的IgG2a同种型。此外，用抗原85A和抗原85B进行鼻内疫苗接种可提供与从鼻内或皮下牛分枝杆菌卡介苗的免疫接种获得的保护相当的保护作用。这些结果表明，通过鼻内途径的粘膜疫苗接种对于结核病疫苗的开发很重要。

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《FEMS immunology and medical microbiology》 |2006年第2期|共9页
作者
Giri PK; Verma I; Khuller GK;
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正文语种 eng
中图分类微生物学;
关键词
Mycobacterium tuberculosis; Vaccination; Vaccines; Proteins; Subcutaneous; 分支杆菌; 结核; 接种; 疫苗; 蛋白质类;

机译：Mycobacterium tuberculosis;Vaccination;Vaccines;Proteins;Subcutaneous;分支杆菌;结核;接种;疫苗;蛋白质类;

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1. Enhanced immunoprotective potential of Mycobacterium tuberculosis Ag85 complex protein based vaccine against airway Mycobacterium tuberculosis challenge following intranasal administration. [J] . Giri PK, Verma I, Khuller GK FEMS immunology and medical microbiology . 2006,第2期

机译：鼻内给药后，结核分枝杆菌基于Ag85复合蛋白的疫苗针对气道结核分枝杆菌攻击的疫苗具有增强的免疫保护潜力。
2. Subcutaneous administration of modified vaccinia virus ankara expressing an AG85B-ESAT6 fusion protein, but not an adenovirus-based vaccine, protects mice against intravenous challenge with Mycobacterium tuberculosis [J] . YouQ., JiangC., WuY., Scandinavian journal of immunology. . 2012,第1期

机译：皮下注射表达AG85B-ESAT6融合蛋白而不是基于腺病毒的疫苗的经修饰的痘苗病毒安卡拉可保护小鼠免受结核分枝杆菌的静脉内攻击
3. Enhancement of tumor-specific T cell-mediated immunity in dendritic cell-based vaccines by mycobacterium tuberculosis heat shock protein X [J] . JungI.D., ShinS.J., LeeM.-G., The Journal of Immunology: Official Journal of the American Association of Immunologists . 2014,第3期

机译：结核分枝杆菌热激蛋白X增强树突状细胞疫苗中肿瘤特异性T细胞介导的免疫
4. Sequence Analysis of the Gene Region Encoding ESAT-6, Ag85B, and Ag85 C Proteins from Clinical Isolates of Mycobacterium tuberculosis [C] . Ni Made Mertaniasih, Didik Handijatno, Agnes Dwi Sis Perwitasari, International Seminar on Molecular and Cellular Life Sciences . 2016

机译：从结核分枝杆菌临床分离株编码ESAT-6，AG85B和AG85 C蛋白的基因区的序列分析
5. Comparison of the efficacy of intranasal versus subcutaneous bacillus calmette-guerin (BCG) vaccination against challenge with virulent Mycobacterium tuberculosis. [D] . Uppari, Sridhar. 2012

机译：鼻内和皮下卡介苗（BCG）接种疫苗对抗强力结核分枝杆菌攻击的功效比较。
6. The Mycobacterium avium subsp. paratuberculosis fibronectin attachment protein a toll-like receptor 4 agonist enhances dendritic cell-based cancer vaccine potency [O] . Kyung Tae Noh, Sung Jae Shin, Kwang Hee Son, 2012

机译：鸟分枝杆菌亚种。肺结核旁纤连蛋白附着蛋白toll样受体4激动剂增强基于树突细胞的癌症疫苗效力
7. Enhanced immunoprotective potential ofMycobacterium tuberculosisAg85 complex protein based vaccine against airwayMycobacterium tuberculosischallenge following intranasal administration [O] . Pramod K. Giri, Indu Verma, Gopal K. Khuller 2006

机译：在鼻内给药后，增强了肺结核菌的免疫保护性潜力对气道结核病的气道肺结核明蛋白疫苗

Enhanced immunoprotective potential of Mycobacterium tuberculosis Ag85 complex protein based vaccine against airway Mycobacterium tuberculosis challenge following intranasal administration.

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