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静脉注射卡介苗和雾化卡介苗再接种可诱导对分枝杆菌有反应的γδ T细胞,其与针对攻击的保护效力相关。

IV BCG Vaccination and Aerosol BCG Revaccination Induce Mycobacteria-Responsive γδ T Cells Associated with Protective Efficacy against Challenge.

作者信息

Morrison Alexandra L, Sarfas Charlotte, Sibley Laura, Williams Jessica, Mabbutt Adam, Dennis Mike J, Lawrence Steve, White Andrew D, Bodman-Smith Mark, Sharpe Sally A

机构信息

Vaccine Development and Evaluation Centre, UK Health Security Agency, Porton Down, Salisbury SP4 0JG, UK.

Infection and Immunity Research Institute, St. George's University of London, London SW17 0BD, UK.

出版信息

Vaccines (Basel). 2023 Oct 17;11(10):1604. doi: 10.3390/vaccines11101604.

Abstract

Intravenously (IV) delivered BCG provides superior tuberculosis (TB) protection compared with the intradermal (ID) route in non-human primates (NHPs). We examined how γδ T cell responses changed in vivo after IV BCG vaccination of NHPs, and whether these correlated with protection against aerosol challenge. In the circulation, Vδ2 T cell populations expanded after IV BCG vaccination, from a median of 1.5% (range: 0.8-2.3) of the CD3+ population at baseline, to 5.3% (range: 1.4-29.5) 4 weeks after , and were associated with TB protection. This protection was related to effector and central memory profiles; homing markers; and production of IFN-γ, TNF-α and granulysin. In comparison, Vδ2 cells did not expand after ID BCG, but underwent phenotypic and functional changes. When Vδ2 responses in bronchoalveolar lavage (BAL) samples were compared between routes, IV BCG vaccination resulted in highly functional mucosal Vδ2 cells, whereas ID BCG did not. We sought to explore whether an aerosol BCG boost following ID BCG vaccination could induce a γδ profile comparable to that induced with IV BCG. We found evidence that the aerosol BCG boost induced significant changes in the Vδ2 phenotype and function in cells isolated from the BAL. These results indicate that Vδ2 population frequency, activation and function are characteristic features of responses induced with IV BCG, and the translation of responses from the circulation to the site of infection could be a limiting factor in the response induced following ID BCG. An aerosol boost was able to localise activated Vδ2 populations at the mucosal surfaces of the lung. This vaccine strategy warrants further investigation to boost the waning human ID BCG response.

摘要

与皮内注射(ID)途径相比,静脉注射(IV)卡介苗在非人灵长类动物(NHP)中提供了更好的结核病(TB)保护。我们研究了NHP静脉注射卡介苗后体内γδ T细胞反应如何变化,以及这些变化是否与抗气溶胶攻击的保护作用相关。在循环系统中,静脉注射卡介苗后Vδ2 T细胞群体扩增,从基线时CD3 +群体的中位数1.5%(范围:0.8 - 2.3)增至4周后的5.3%(范围:1.4 - 29.5),且与结核病保护相关。这种保护与效应器和中央记忆表型、归巢标志物以及IFN - γ、TNF - α和颗粒溶素的产生有关。相比之下,皮内注射卡介苗后Vδ2细胞未扩增,但发生了表型和功能变化。当比较不同途径支气管肺泡灌洗(BAL)样本中的Vδ2反应时,静脉注射卡介苗导致黏膜Vδ2细胞具有高度功能,而皮内注射卡介苗则不然。我们试图探索皮内注射卡介苗后进行气溶胶卡介苗加强免疫是否能诱导出与静脉注射卡介苗相当的γδ表型。我们发现有证据表明,气溶胶卡介苗加强免疫在从BAL中分离的细胞中诱导了Vδ2表型和功能的显著变化。这些结果表明,Vδ2群体频率、激活和功能是静脉注射卡介苗诱导反应的特征,并且从循环系统到感染部位的反应转化可能是皮内注射卡介苗后诱导反应的限制因素。气溶胶加强免疫能够将活化的Vδ2群体定位在肺部黏膜表面。这种疫苗策略值得进一步研究,以增强逐渐减弱的人皮内注射卡介苗反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5f3d/10611416/39931443d040/vaccines-11-01604-g001.jpg

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