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首页> 外文期刊>European journal of pharmaceutical sciences >Improved protection against tuberculosis after boosting the BCG-primed mice with subunit Ag 85a delivered through intact skin with deformable vesicles
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Improved protection against tuberculosis after boosting the BCG-primed mice with subunit Ag 85a delivered through intact skin with deformable vesicles

机译:用带有可变形囊泡的完整皮肤递送的具有亚基Ag 85a的BCG初免小鼠加强了对结核病的保护

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To improve vaccination against tuberculosis (TBC) with Bacillus Calmette-Guerin (BCG), we introduce novel, non-invasive, secondary immunisations relying on epicutaneous (e.c.) applications of the TBC subunit antigen, Ag 85a, associated with deformable carrier vesicles. Immuno-boosting with such antigen-vesicles recruits more CD11c positive cells into the draining murine lymph nodes, and typically stimulates, especially the proximal, immune cells more than immunogen injections. Non-invasive antigen application also protects mice better against an infection with TBC. Subcutaneous injections of vesicular Ag 85a into BCG-primed mice mainly yield IgG1 and IgG2a, indicative of a mixed Th1 and Th2 response. Conversely, transcutaneous immuno-boosts of such mice with a deformable vesicle-Ag 85a combination mainly generate serum IgA and IgG2a, indicative of an IgA facilitated, Th1-mediated, immune response. The Ag 85a specific antibody titres are generally low, but T lymphocytes also proliferate in the immunised mice. The new, partially non-invasive, vaccination method lowers the burden of pulmonary infection with M. tuberculosis. In mice immunised with Ag85a associated with deformable vesicles we measured 116x (e.c.) to 51x (s.c.) lower colony forming units number in spleen and 9x (e.c.) to 3x (s.c.) lower such number in lungs. (C) 2015 Elsevier B.V. All rights reserved.
机译:为了改善卡介苗芽孢杆菌(BCG)的结核病(TBC)疫苗接种,我们引入了依赖于TBC亚基抗原Ag 85a的表皮(e.c.)应用与可变形载体囊泡相关的新型非侵入性二次免疫。通过这种抗原小泡的免疫增强将更多的CD11c阳性细胞募集到引流的小鼠淋巴结中,并且通常比免疫原注射更多地刺激(尤其是近端)免疫细胞。非侵入性抗原的应用还可以更好地保护小鼠免受TBC感染。向BCG引发的小鼠皮下注射囊泡Ag 85a主要产生IgG1和IgG2a,表明Th1和Th2混合反应。相反,具有可变形囊泡-Ag 85a组合的此类小鼠的经皮免疫增强剂主要产生血清IgA和IgG2a,表明IgA促进了Th1介导的免疫反应。 Ag 85a特异性抗体的效价通常很低,但T淋巴细胞也在免疫小鼠中增殖。新的,部分非侵入性的疫苗接种方法减轻了结核分枝杆菌的肺部感染负担。在用与可变形囊泡相关的Ag85a免疫的小鼠中,我们测量的脾脏集落形成单位数降低了116x(e.c.)至51x(s.c.),而肺部降低了9x(e.c.)至3x(s.c.)。 (C)2015 Elsevier B.V.保留所有权利。

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