首页> 外文期刊>The Journal of Allergy and Clinical Immunology >Der p 1 peptide on virus-like particles is safe and highly immunogenic in healthy adults.
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Der p 1 peptide on virus-like particles is safe and highly immunogenic in healthy adults.

机译:在健康成年人中,病毒样颗粒上的Der p 1肽是安全的且具有高度免疫原性。

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BACKGROUND: In mice, highly repetitive antigens, such as those present on bacterial or viral surfaces, efficiently cross-link B-cell receptors and therefore induce strong IgG responses. In this study we covalently coupled a synthetic 16-amino-acid sequence of the allergen Der p 1 to a virus-like particle derived from the bacteriophage Qbeta (Qbeta-Der p 1). OBJECTIVE: We evaluated the safety and immunogenicity of Qbeta-Der p 1 in human subjects and compared different doses and routes of immunization. METHODS: In a phase I trial 24 healthy volunteers were randomly assigned to one of 4 treatment groups. Group 1 received 50 microg of Qbeta-Der p 1 intramuscularly, group 2 received 50 microg of Qbeta-Der p 1 subcutaneously, group 3 received 10 microg of Qbeta-Der p 1 intramuscularly, and group 4 received 10 microg of Qbeta-Der p 1 subcutaneously. Boosting immunizations with 10 microg were given after 1 and 3 months. Antibody titers were measured after 1, 3, 4, 6, 12, and 18 months. RESULTS: The vaccine Qbeta-Der p 1 was well tolerated. Significant IgG responses were observed 4 weeks after a single injection. Individuals receiving 50 microg of the vaccine had significantly higher IgG titers than those vaccinated with 10 microg. However, the route of immunization (subcutaneous vs intramuscular) had no effect. In the 50-microg dose group, strong antibody responses against Der p 1 with average titers of 1:2000 were obtained. CONCLUSION: Vaccination with a peptide antigen covalently coupled to highly repetitive virus-like particles represents an adjuvant-free means of rapidly inducing high antibody titers in human subjects. CLINICAL IMPLICATIONS: Allergens coupled to virus-like particles can be used to enhance the efficiency of allergen-specific immunotherapy.
机译:背景:在小鼠中,高度重复的抗原(例如存在于细菌或病毒表面的抗原)可以有效地交联B细胞受体,从而诱导强烈的IgG反应。在这项研究中,我们将变应原Der p 1的合成16个氨基酸序列与衍生自噬菌体Qbeta(Qbeta-Der p 1)的病毒样颗粒共价偶联。目的:我们评估了Qbeta-Der p 1在人类受试者中的安全性和免疫原性,并比较了不同剂量和免疫途径。方法:在I期试验中,将24名健康志愿者随机分配到4个治疗组之一中。第1组肌内接受50微克Qbeta-Der p 1,第2组肌内接受50微克Qbeta-Der p 1,第3组肌内接受10微克Qbeta-Der p 1,第4组接受10微克Qbeta-Der p 1。 1皮下。在1和3个月后,用10微克加强免疫。在1、3、4、6、12和18个月后测量抗体滴度。结果:疫苗Qbeta-Der p 1被很好地耐受。单次注射后4周观察到明显的IgG反应。接种50微克疫苗的人的IgG滴度明显高于接种10微克疫苗的人。但是,免疫途径(皮下与肌内)均无效。在50微克剂量组中,获得了针对Der p 1的强抗体反应,平均效价为1:2000。结论:与高重复性病毒样颗粒共价偶联的肽抗原疫苗接种代表了无佐剂,可在人受试者中快速诱导高抗体滴度。临床意义:过敏原与病毒样颗粒偶联可用于提高过敏原特异性免疫疗法的效率。

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