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Enhanced Immunogenicity of Plasmodium falciparum Peptide Vaccines Using a Topical Adjuvant Containing a Potent Synthetic Toll-Like Receptor 7 Agonist, Imiquimod ▿

机译:使用含有强效合成Toll样受体7激动剂Imiquimod的局部佐剂增强恶性疟原虫肽疫苗的免疫原性

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摘要

Plasmodium sporozoites injected into the skin by malaria-infected mosquitoes can be effectively targeted by antibodies that block parasite invasion of host hepatocytes and thus prevent the subsequent development of blood stage infections responsible for clinical disease. Malaria subunit vaccines require potent adjuvants, as they lack known pathogen-associated molecular patterns found in attenuated viral or bacterial vaccines that function as Toll-like receptor (TLR) agonists to stimulate dendritic cells and initiate strong adaptive immune responses. A synthetic TLR7 agonist, imiquimod, which is FDA approved for topical treatment of various skin conditions, can function as a potent adjuvant for eliciting T-cell responses to intracellular pathogens and model protein antigens. In the current studies, the topical application of imiquimod at the site of subcutaneously injected Plasmodium falciparum circumsporozoite (CS) peptides elicited strong parasite-specific humoral immunity that protected against challenge with transgenic rodent parasites that express P. falciparum CS repeats. In addition, injection of a simple linear peptide followed by topical imiquimod elicited strong Th1 CD4+ T-cell responses, as well as high antibody titers. The correlation of high anti-repeat antibody titers with resistance to sporozoite challenge in vivo and in vitro supports use of this topical TLR7 agonist adjuvant to elicit protective humoral immunity. The safety, simplicity, and economic advantages of a topical synthetic TLR7 agonist adjuvant also apply to other vaccines requiring high antibody titers, such as malaria asexual or sexual blood stage antigens to prevent red blood cell invasion and block transmission to the mosquito vector, and to vaccines to other extracellular pathogens.
机译:疟疾感染的蚊子注射到皮肤中的疟原虫子孢子可以被抗体有效地靶向,这些抗体可以阻止寄生虫入侵宿主肝细胞,从而阻止随后发展为临床疾病的血液阶段感染。疟疾亚单位疫苗需要有效的佐剂,因为它们缺乏在减毒的病毒或细菌疫苗中发现的与病原体相关的分子模式,这种模式可充当Toll样受体(TLR)激动剂来刺激树突状细胞并启动强烈的适应性免疫反应。 FDA批准用于各种皮肤病的局部治疗的合成TLR7激动剂咪喹莫特,可作为有效的佐剂,引起对细胞内病原体和模型蛋白抗原的T细胞反应。在当前的研究中,在皮下注射恶性疟原虫环子孢子(CS)肽的部位局部应用咪喹莫特引起了强烈的寄生虫特异性体液免疫,该免疫力可抵抗表达恶性疟原虫CS重复序列的转基因啮齿动物寄生虫的攻击。此外,注射简单的线性肽,然后局部用咪喹莫特引起强烈的Th1 CD4 + T细胞反应,以及高抗体滴度。高抗重复抗体滴度与体内和体外对子孢子攻击的抗性之间的相关性支持使用该局部TLR7激动剂佐剂引起保护性体液免疫。局部合成TLR7激动剂佐剂的安全性,简便性和经济优势也适用于其他需要高抗体滴度的疫苗,例如疟疾无性或性血液阶段抗原,以防止红细胞入侵并阻止向蚊媒的传播。其他细胞外病原体的疫苗。

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