Coxevac® is the EMA-approved veterinary vaccine for the protection of cattle and goats against Q fever, a zoonotic bacterial disease due to Coxiella burnetii. Since Coxevac® reduces bacterial shedding and clinical symptoms but does not prevent infection, novel, ready-to-use vaccine formulations are needed to increase its immunogenicity. Here, a goat vaccination-challenge model was used to evaluate the impact of the commercially available saponin-based QuilA® adjuvant on Coxevac® immunity. Upon challenge, the QuilA®-Coxevac® group showed a stronger immune response reflected in a higher magnitude of total IgG and an increase in circulating and splenic CD8(+) T-cells compared to the Coxevac® and challenged-control groups. The QuilA®-Coxevac® group was characterized by a targeted Th1-type response (IFNγ, IP10) associated with increased transcripts of CD8(+) and NK cells in spleens and γδ T cells in bronchial lymph nodes. Coxevac® vaccinated animals presented an intermediate expression of Th1-related genes, while the challenged-control group showed an immune response characterized by pro-inflammatory (IL1β, TNFα, IL12), Th2 (IL4 and IL13), Th17 (IL17A) and other immunoregulatory cytokines (IL6, IL10). An intriguing role was observed for γδ T cells, which were of TBX21- and SOX4-types in the QuilA®-Coxevac® and challenged control group, respectively. Overall, the addition of QuilA® resulted in a sustained Th1-type activation associated with an increased vaccine-induced bacterial clearance of 33.3% as compared to Coxevac® only. QuilA® could be proposed as a readily-applied veterinary solution to improve Coxevac® efficacy against C. burnetii infection in field settings.
QuilA® adjuvanted Coxevac® sustains Th1-CD8(+)-type immunity and increases protection in Coxiella burnetii-challenged goats.
QuilA®佐剂Coxevac®可维持Th1-CD8(+)型免疫力,并增强对感染伯氏考克斯体(Coxiella burnetii)的山羊的保护作用
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作者:Tomaiuolo Sara, Jansen Wiebke, Soares Martins Susana, Devriendt Bert, Cox Eric, Mori Marcella
| 期刊: | NPJ Vaccines | 影响因子: | 6.500 |
| 时间: | 2023 | 起止号: | 2023 Feb 14; 8(1):17 |
| doi: | 10.1038/s41541-023-00607-z | 靶点: | CD8 |
| 研究方向: | 免疫/内分泌 | ||
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