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体外人CD4 + T细胞对痘苗保护性抗原B5R和A33R的反应。

In vitro human CD4+ T cell response to the vaccinia protective antigens B5R and A33R.

作者信息

Sirven Philemon, Castelli Florence Anne, Probst Alicia, Szely Natacha, Maillere Bernard

机构信息

CEA, iBiTecS, Service d'Ingénierie Moléculaire des Protéines (SIMOPRO), Gif Sur Yvette F-91191, France.

出版信息

Mol Immunol. 2009 Apr;46(7):1481-7. doi: 10.1016/j.molimm.2008.12.016. Epub 2009 Feb 3.

Abstract

Subunit vaccine candidates against poxvirus infection induced protective humoral and cellular response in animal models but their immunogenicity in human remains unknown. We have therefore evaluated in vitro the CD4 T cell response of the major antigens B5R and A33R and characterized their CD4 T cell epitopes. Twelve peptides selected on the basis of their binding capacity to HLA-DR molecules, induced CD4 T lymphocytes harvested in healthy donors. In the A33R proteins two peptides are T cell stimulating for at least half of the donors and are restricted to multiple HLA-DR molecules in agreement with their broad specificity for HLA-DR molecules. In B5R, two peptides exhibited a good immunoprevalence but only one is a good binder to multiple HLA-DR molecules. One peptide was a moderate binder for multiple HLA-DR molecules, although it was efficiently presented to peptide-specific T cell lines. Altogether, our data demonstrated the capacity of B5R and A33R peptides to elicit a T cell response in multiple healthy donors and showed that promiscuity and immunoprevalence of CD4 T cell epitopes are not necessarily associated.

摘要

针对痘病毒感染的亚单位疫苗候选物在动物模型中诱导了保护性体液和细胞反应,但其在人类中的免疫原性尚不清楚。因此,我们在体外评估了主要抗原B5R和A33R的CD4 T细胞反应,并对其CD4 T细胞表位进行了表征。根据与HLA-DR分子的结合能力选择的12种肽,诱导了从健康供体中收获的CD4 T淋巴细胞。在A33R蛋白中,两种肽对至少一半的供体具有T细胞刺激作用,并与它们对HLA-DR分子的广泛特异性一致,受多种HLA-DR分子限制。在B5R中,两种肽表现出良好的免疫流行率,但只有一种是与多种HLA-DR分子的良好结合物。一种肽是与多种HLA-DR分子的中度结合物,尽管它能有效地呈递给肽特异性T细胞系。总之,我们的数据证明了B5R和A33R肽在多个健康供体中引发T细胞反应的能力,并表明CD4 T细胞表位的多反应性和免疫流行率不一定相关。

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