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Two Studies Evaluating the Safety and Immunogenicity of a Live, Attenuated Shigella flexneri 2a Vaccine (SC602) and Excretion of Vaccine Organisms in North American Volunteers

机译:两项评估北美志愿人员减毒的志贺氏菌2a活疫苗(SC602)的安全性和免疫原性以及疫苗生物排泄的两项研究

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摘要

We report the first community-based evaluation of Shigella flexneri 2a strain SC602, a live, oral vaccine strain attenuated by deletion of the icsA (virG) plasmid virulence gene, given at 104 CFU. The primary objectives of this trial were to determine the safety and immunogenicity of the vaccine and to determine the duration of colonization. Four of 34 volunteers experienced transient fevers, and three reported diarrhea during the first 3 days of the study. Half of the volunteers mounted a positive serum immunoglobulin A (IgA) response to S. flexneri lipopolysaccharide. All but one of the volunteers excreted the vaccine in their stools for 1 to 33 days, and this excretion was often intermittent. Data from the community-based study were supplemented with an inpatient trial in which three volunteers received 103 and nine received 104 CFU. All volunteers who received 103 CFU excreted SC602 and had an IgA antibody-secreting cell response. Two of these had a serum IgA response. Six of the nine volunteers who received 104 CFU excreted SC602. One vaccinee had a transient fever and two met the definition of diarrhea. Six volunteers that received 104 CFU had an antibody-secreting cell response, and four had a serum IgA response. SC602 has now been tested at 104 CFU in a total of 58 volunteers. The cumulative results of these clinical trials, reported here and previously (Coster et al., Infect. Immun. 67:3437-3443, 1999), have demonstrated that SC602 is a substantially attenuated candidate vaccine that can evoke protection against the most severe symptoms of shigellosis in a stringent human challenge model of disease.
机译:我们报告了志贺氏志贺氏菌2a菌株SC602的首次基于社区的评估,这是一种通过删除icsA(virG)质粒毒力基因而引起的减毒活疫苗,在104 CFU给予。该试验的主要目的是确定疫苗的安全性和免疫原性,并确定定植时间。在研究的前3天中,有34名志愿者中有4名经历了短暂发烧,其中3名报告了腹泻。一半的志愿者对弗氏链球菌脂多糖表现出阳性的血清免疫球蛋白A(IgA)反应。除一名志愿者外,所有志愿者都在粪便中排泄了疫苗1至33天,并且这种排泄通常是间歇性的。来自社区研究的数据得到了住院试验的补充,其中三名志愿者接受了103 CFU,九名接受了104 CFU。接受103 CFU的所有志愿者均分泌SC602,并分泌IgA抗体。其中两个有血清IgA反应。接受104 CFU的9位志愿者中有6位排泄了SC602。一名疫苗接种者出现短暂发烧,其中两名达到腹泻的定义。接受104 CFU的六名志愿者发生了分泌抗体的细胞反应,其中四名发生了血清IgA反应。 SC602现在已经在104位CFU上对58位志愿者进行了测试。这些临床试验的累积结果,如此处和之前所报道(Coster等,Infect。Immun。67:3437-3443,1999),已证明SC602是一种实质上减毒的候选疫苗,可以引起针对最严重症状的保护作用严峻的人类疾病挑战模型中的志贺菌病。

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