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编码幽门螺杆菌脲酶B亚基的脊髓灰质炎病毒复制子引发Th1相关免疫反应。

Poliovirus replicons encoding the B subunit of Helicobacter pylori urease elicit a Th1 associated immune response.

作者信息

Novak M J, Smythies L E, McPherson S A, Smith P D, Morrow C D

机构信息

Department of Microbiology, University of Alabama at Birmingham 35294, USA.

出版信息

Vaccine. 1999 May 14;17(19):2384-91. doi: 10.1016/s0264-410x(99)00035-3.

Abstract

The development of a vaccine for Helicobacter pylori is a key strategy for reducing the worldwide prevalence of H. pylori infection. Although immunization with recombinant B subunit of H. pylori urease (ureB) has yielded promising results, for the most part, these studies relied on the use of strong adjuvant, cholera toxin, precluding the use in humans. Thus, the development of new vaccine strategies for H. pylori is essential. Previous studies from our laboratory have described a vaccine vector based on poliovirus in which foreign genes are substituted for the poliovirus capsid genes. The genomes encoding foreign proteins (replicons) are encapsidated into authentic poliovirions by providing the capsids in trans. To test the utility of replicons as a vaccine vector for H. pylori, a replicon was constructed which encodes ureB. Expression of ureB in cells from the replicon was demonstrated by metabolic labeling followed by immunoprecipitation with anti-urease antibodies. To investigate the immunogenicity of the replicons, mice containing the transgene for the receptor for poliovirus were immunized via the intramuscular route. Mice given three doses of replicons did not develop substantial antibodies to ureB as determined by Western blot analysis using lysates from H. pylori. In contrast, mice given two doses of replicon followed by a single injection of recombinant ureB developed serum antibodies to ureB which were predominately IgG2a. Splenic lymphocytes from mice immunized with replicons alone, or replicons plus recombinant ureB produced abundant interferon-gamma and no detectable interleukin-4 upon stimulation with recombinant ureB. These results establish that poliovirus replicons encoding H. pylori ureB are immunogenic and induce primarily a T helper 1 associated immune response.

摘要

开发幽门螺杆菌疫苗是降低全球幽门螺杆菌感染率的关键策略。尽管用幽门螺杆菌脲酶重组B亚基(ureB)进行免疫已取得了有前景的结果,但在很大程度上,这些研究依赖于使用强佐剂霍乱毒素,这排除了其在人体中的应用。因此,开发新的幽门螺杆菌疫苗策略至关重要。我们实验室之前的研究描述了一种基于脊髓灰质炎病毒的疫苗载体,其中外源基因取代了脊髓灰质炎病毒衣壳基因。通过反式提供衣壳,将编码外源蛋白的基因组(复制子)包装到正宗的脊髓灰质炎病毒颗粒中。为了测试复制子作为幽门螺杆菌疫苗载体的效用,构建了一个编码ureB的复制子。通过代谢标记,然后用抗脲酶抗体进行免疫沉淀,证明了复制子在细胞中ureB的表达。为了研究复制子的免疫原性,对含有脊髓灰质炎病毒受体转基因的小鼠进行肌肉注射免疫。通过使用幽门螺杆菌裂解物进行蛋白质印迹分析确定,给予三剂复制子的小鼠没有产生大量针对ureB的抗体。相比之下,给予两剂复制子然后单次注射重组ureB的小鼠产生了针对ureB的血清抗体,这些抗体主要是IgG2a。单独用复制子或复制子加重组ureB免疫的小鼠的脾淋巴细胞在用重组ureB刺激后产生大量干扰素-γ,未检测到白细胞介素-4。这些结果表明,编码幽门螺杆菌ureB的脊髓灰质炎病毒复制子具有免疫原性,并主要诱导与T辅助1相关的免疫反应。

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