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Priming with an Adenovirus 35-Circumsporozoite Protein (CS) Vaccine followed by RTSS/AS01B Boosting Significantly Improves Immunogenicity to Plasmodium falciparum CS Compared to That with Either Malaria Vaccine Alone

机译：与单独使用疟疾疫苗相比先用腺病毒35-环子孢子蛋白（CS）疫苗再加上RTSS / AS01B进行初次免疫可显着提高对恶性疟原虫CS的免疫原性

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The RTS,S/AS02A protein-based vaccine consistently demonstrates significant protection against infection with Plasmodium falciparum malaria and also against clinical malaria and severe disease in children in areas of endemicity. Here we demonstrate with rhesus macaques that priming with a replication-defective human adenovirus serotype 35 (Ad35) vector encoding circumsporozoite protein (CS) (Ad35.CS), followed by boosting with RTS,S in an improved MPL- and QS21-based adjuvant formulation, AS01B, maintains antibody responses and dramatically increases levels of T cells producing gamma interferon and other Th1 cytokines in response to CS peptides. The increased T-cell responses induced by the combination of Ad35.CS and RTS,S/AS01B are sustained for at least 6 months postvaccination and may translate to improved and more durable protection against P. falciparum infection in humans.

机译：基于RTS，S / AS02A的蛋白质疫苗始终显示出对流行性地区儿童恶性疟原虫疟疾感染以及临床疟疾和严重疾病的有效保护。在这里，我们用恒河猴证明，用编码环子孢子蛋白（CS）（Ad35.CS）的复制缺陷型人类腺病毒血清型35（Ad35）载体引发，然后在改良的基于MPL和QS21的佐剂中用RTS，S加强免疫AS01B制剂可维持抗体应答，并显着增加响应CS肽的T细胞产生γ干扰素和其他Th1细胞因子的水平。疫苗接种后，Ad35.CS和RTS，S / AS01B的组合诱导的T细胞应答增加可持续至少6个月，并可能转化为对人类恶性疟原虫感染的改良且更持久的保护。

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期刊名称 Infection and Immunity
作者
V. Ann Stewart; Shannon M. McGrath; Patrice M. Dubois; Maria G. Pau; Pascal Mettens; Joseph Shott; Michelle Cobb; J. Robert Burge; David Larson; Lisa A. Ware; Marie-Ange Demoitie; Gerrit Jan Weverling; Babak Bayat; Jerome H. H. V. Custers; Marie-Claude Dubois; Joe Cohen; Jaap Goudsmit; D. Gray Heppner Jr.;
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年(卷),期 2007(75),5
年度 2007
页码 2283–2290
总页数 8
原文格式 PDF
正文语种
中图分类免疫学;病毒传染病;
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专利

1. Priming with an Adenovirus 35-Circumsporozoite Protein (CS) Vaccine followed by RTS,S/AS01B Boosting Significantly Improves Immunogenicity to Plasmodium falciparum CS Compared to That with Either Malaria Vaccine Alone [J] . V. Ann Stewart, Shannon M. McGrath, Patrice M. Dubois, Infection and immunity . 2007,第5期

机译：与单独使用疟疾疫苗相比，先用腺病毒35-环子孢子蛋白（CS）疫苗再加上RTS，S / AS01B进行初次免疫可显着提高对恶性疟原虫CS的免疫原性
2. Human adenovirus 5-vectored Plasmodium falciparum NMRC-M3V-Ad-PfCA vaccine encoding CSP and AMA1 is safe, well-tolerated and immunogenic but does not protect against controlled human malaria infection [J] . Tamminga Cindy, Sedegah Martha, Maiolatesi Santina, Human vaccines & immunotherapeutics. . 2013,第10期

机译：人腺病毒5载体恶性疟原虫NMRC-M3V-Ad-PfCA编码CSP和AMA1的疫苗是安全，耐受性良好和具有免疫原性的疫苗，但不能预防人类疟疾的感染
3. Clinical trial in healthy malaria-na?ve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA [J] . RichieT.L., CharoenvitY., WangR., Human vaccines & immunotherapeutics. . 2012,第11期

机译：在未患疟疾的健康成年人中进行临床试验，以评估MuStDO5的安全性，耐受性，免疫原性和功效，MuStDO5是一种五基因子孢子/肝阶段恶性疟原虫DNA疫苗，并逐步增加剂量的人GM-CSF DNA
4. Immunogenicity of Malaria Vaccine Candidate-Plasmodium falciparum Merozoite Surface Protein 5 (PfMSP5) Expressed in Bacillus subtilis [C] . Chittibabu Gottimukkala, Charles Ma, Hans J. Netter International Conference on Chemical, Biological and Environmental Engineering . 2014

机译：疟疾疫苗候选疟原虫的免疫原性是恶魔植物在枯草芽孢杆菌中表达的疟原虫候选疟原虫疟原虫表面蛋白5（PFMSP5）
5. Analysis of human immune responses to malaria vaccines containing a universal T helper epitope of Plasmodium falciparum CS protein. [D] . Calvo-Calle, Jaime Mauricio. 2004

机译：人类对疟疾疫苗的免疫反应分析，该疫苗含有恶性疟原虫CS蛋白的通用T辅助表位。
6. Human adenovirus 5-vectored Plasmodium falciparum NMRC-M3V-Ad-PfCA vaccine encoding CSP and AMA1 is safe well-tolerated and immunogenic but does not protect against controlled human malaria infection [O] . Cindy Tamminga, Martha Sedegah, Santina Maiolatesi, 2013

机译：人腺病毒5载体恶性疟原虫NMRC-M3V-Ad-PfCA编码CSP和AMA1的疫苗是安全耐受性良好和具有免疫原性的疫苗但不能预防人类疟疾的感染
7. Priming with an Adenovirus 35-Circumsporozoite Protein (CS) Vaccine followed by RTS,S/AS01B Boosting Significantly Improves Immunogenicity to Plasmodium falciparum CS Compared to That with Either Malaria Vaccine Alone▿ [O] . Stewart, V. Ann, McGrath, Shannon M., Dubois, Patrice M., 2007

机译：与单独使用疟疾疫苗相比，先用腺病毒35-环子孢子蛋白（CS）疫苗进行初次接种，然后再进行RTS，S / AS01B增强，可显着提高对恶性疟原虫CS的免疫原性。
8. DNA Prime/Adenovirus Boost Malaria Vaccine Encoding P. falciparum CSP and AMA1 Induces Sterile Protection Associated with Cell-Mediated Immunity. [R] . I. Chuang M. Polhemus M. Sedegah M. Spring S. Cicatelli 2013

机译：DNa prime / adenovirus Boost疟疾疫苗编码恶性疟原虫Csp和ama1诱导与细胞介导的免疫相关的无菌保护。

Priming with an Adenovirus 35-Circumsporozoite Protein (CS) Vaccine followed by RTSS/AS01B Boosting Significantly Improves Immunogenicity to Plasmodium falciparum CS Compared to That with Either Malaria Vaccine Alone

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