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HIV-1 vaccine strategies utilizing viral vectors including antigen-displayed inoviral vectors

机译:利用病毒载体(包括抗原展示的病毒载体)的HIV-1疫苗策略

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Antigen-presenting viral vectors have been extensively used as vehicles for the presentation of antigens to the immune system in numerous vaccine strategies. Particularly in HIV vaccine development efforts, two main viral vectors have been used as antigen carriers: (a) live attenuated vectors and (b) virus-like particles (VLPs); the former, although highly effective in animal studies, cannot be clinically tested in humans due to safety concerns and the latter have failed to induce broadly neutralizing anti-HIV antibodies. For more than two decades, Inoviruses (non-lytic bacterial phages) have also been utilized as antigen carriers in several vaccine studies. Inoviral vectors are important antigen-carriers in vaccine development due to their ability to present an antigen on their outer architecture in many copies and to their natural high immunogenicity. Numerous fundamental studies have been conducted, which have established the unique properties of antigen-displayed inoviral vectors in HIV vaccine efforts. The recent isolation of new, potent anti-HIV broadly neutralizing monoclonal antibodies provides a new momentum in this emerging technology.
机译:呈递抗原的病毒载体已被广泛用作许多疫苗策略中向免疫系统呈递抗原的载体。特别是在HIV疫苗开发工作中,两种主要的病毒载体已被用作抗原载体:(a)减毒活载体和(b)病毒样颗粒(VLP);前者尽管在动物研究中非常有效,但出于安全考虑,无法在人体中进行临床测试,而后者未能诱导广泛中和的抗HIV抗体。在超过二十年的时间里,猪流感病毒(非溶菌噬菌体)也已被用作疫苗研究的抗原载体。病毒载体是疫苗开发中重要的抗原载体,这是由于它们能够以许多拷贝在其外部结构上呈递抗原的能力以及其天然的高免疫原性。已经进行了许多基础研究,这些研究已经确定了抗原展示的病毒载体在HIV疫苗研发中的独特性能。最近分离出的新的,有效的抗HIV广泛中和单克隆抗体为这项新兴技术提供了新的动力。

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