首页> 美国卫生研究院文献>Frontiers in Immunology >Gut-Homing Conventional Plasmablasts and CD27− Plasmablasts Elicited after a Short Time of Exposure to an Oral Live-Attenuated Shigella Vaccine Candidate in Humans
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Gut-Homing Conventional Plasmablasts and CD27− Plasmablasts Elicited after a Short Time of Exposure to an Oral Live-Attenuated Shigella Vaccine Candidate in Humans

机译:短时间暴露于人类口服活检志贺氏菌疫苗候选者后肠归巢的常规等离子母细胞和CD27-等离子母细胞被激发

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摘要

Currently, there is no licensed Shigella vaccine; however, various promising live-attenuated vaccine candidates have emerged, including CVD1208S (ΔguaBA, Δset, Δsen S. flexneri 2a), which was shown to be safe and immunogenic in Phase 1 clinical trials. Here, we report the immune responses elicited in an outpatient Phase 2 clinical trial in which subjects were vaccinated with CVD 1208S. Oral immunization with CVD 1208S elicited high anti-S. flexneri 2a LPS and IpaB antibody responses as well as an acute plasmablast (PB) infiltration in peripheral blood 7 days after immunization. PB sorted based on their expression of homing molecules confirmed that cells expressing integrin α4β7 alone or in combination with CD62L were responsible for antibody production (as measured by ELISpot). Furthermore, using high-color flow-cytometry, on day 7 after immunization, we observed the appearance of conventional PB (CPB, CD19dim CD20 CD27+high CD38+high CD3), as well as a PB population that did not express CD27 (CD27 PB; pre-plasmablasts). The pattern of individual or simultaneous expression of homing markers (integrin α4β7, CD62L, CXCR3, and CXCR4) suggested that CPB cells homed preferentially to the inflamed gut mucosa. In contrast, ~50% CD27 PB cells appear to home to yet to be identified peripheral lymphoid organs or were in a transition state preceding integrin α4β7 upregulation. In sum, these observations demonstrate that strong immune responses, including distinct PB subsets with the potential to home to the gut and other secondary lymphoid organs, can be elicited after a short time of exposure to a shigella oral vaccine.
机译:当前,没有许可的志贺氏菌疫苗;然而,已经出现了多种有希望的减毒活疫苗候选物,包括CVD1208S(ΔguaBA,Δset,ΔsenS. flexneri 2a),在1期临床试验中已证明是安全且具有免疫原性的。在这里,我们报告了在门诊2期临床试验中引起的免疫反应,在该试验中,受试者已接种CVD 1208S疫苗。用CVD 1208S进行口服免疫可产生高抗-S。免疫后7天,flexneri 2a LPS和IpaB抗体反应以及外周血中的急性浆母细胞(PB)浸润。根据归巢分子的表达分类的PB证实,单独表达整联蛋白α4β7或与CD62L结合表达整联蛋白α4β7的细胞负责抗体的产生(通过ELISpot测量)。此外,使用高色流式细胞仪,在免疫后第7天,我们观察到了传统PB(CPB,CD19 dim CD20 - CD27 + high CD38 + high CD3 -),以及不表达CD27的PB人群(CD27 - PB;成浆细胞)。归巢标记(整联蛋白α4β7,CD62L,CXCR3和CXCR4)单独或同时表达的模式表明,CPB细胞优先归巢于发炎的肠粘膜。相反,约50%的CD27 - PB细胞似乎归巢于尚未被识别的外周淋巴器官,或者在整合素α4β7上调之前处于过渡状态。总之,这些观察结果表明,在短时间接触志贺氏菌口服疫苗后,可以引起强烈的免疫反应,包括具有居于肠道和其他次级淋巴器官潜能的不同的PB亚群。

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