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Process development for the production of an E. coli produced clinical grade recombinant malaria vaccine for Plasmodium vivax

机译:生产间日疟原虫的大肠杆菌生产的临床级重组疟疾疫苗的工艺开发

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The global eradication of malaria will require the development of vaccines to prevent infection cause by Plasmodium vivax in addition to Plasmodium falciparum. In an attempt to contribute to this effort we have previously reported the cloning and expression of a vaccine based on the circumsporozoite protein of P. vivax. The synthetic vaccine encodes for a full-length molecule encompassing the N-terminal and C-terminal regions flanking a chimeric repeat region representing VK210 and VK247, the two major alleles of P. vivax CSP. The vaccine, designated vivax malaria protein 001 (VMP001), was purified to >95% homogeneity using a three-column purification scheme and had low endotoxin levels and passed the rabbit pyrogenicity assay. The protein is recognized by monoclonal antibodies directed against the two repeat motifs, as well as polyclonal antibodies. Immunization with VMP001 induced high titer antibodies in mice using Montanide ISA 720. We currently have more than 10,000 doses of purified bulk and 1800 vials of formulated bulk vaccine available for clinical testing and VMP001 is currently undergoing further development as a candidate vaccine to prevent malaria in humans.
机译:在全球范围内根除疟疾将需要开发疫苗来预防除恶性疟原虫外还由间日疟原虫引起的感染。为了促进这一努力,我们先前已经报道了一种基于间日疟原虫环子孢子蛋白的疫苗的克隆和表达。合成疫苗编码一个全长分子,该分子包含N端和C端区域,侧翼是代表间日疟原虫CSP的两个主要等位基因VK210和VK247的嵌合重复区。使用三柱纯化方案将疫苗命名为间日疟原虫疟疾蛋白001(VMP001),纯化到> 95%的同质性,且内毒素水平低,并通过了兔热原性检测。该蛋白被针对两个重复基序的单克隆抗体以及多克隆抗体识别。使用Montanide ISA 720在小鼠中免疫VMP001诱导的高滴度抗体。我们目前有10,000多种纯化的散装疫苗和1800瓶配制的散装疫苗可用于临床测试,并且VMP001目前正在作为预防疟疾的候选疫苗进行进一步开发。人类。

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