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人类甲型流感病毒特异性细胞毒性T淋巴细胞反应的强度和特异性与HLA - A和 - B表型有关。

The magnitude and specificity of influenza A virus-specific cytotoxic T-lymphocyte responses in humans is related to HLA-A and -B phenotype.

作者信息

Boon A C M, de Mutsert G, Graus Y M F, Fouchier R A M, Sintnicolaas K, Osterhaus A D M E, Rimmelzwaan G F

机构信息

Institute of Virology, Erasmus University Rotterdam, 3015 GE Rotterdam, The Netherlands.

出版信息

J Virol. 2002 Jan;76(2):582-90. doi: 10.1128/jvi.76.2.582-590.2002.

Abstract

The repertoire of human cytotoxic T-lymphocytes (CTL) in response to influenza A viruses has been shown to be directed towards multiple epitopes, with a dominant response to the HLA-A2-restricted M1(58-66) epitope. These studies, however, were performed with peripheral blood mononuclear cells (PBMC) of individuals selected randomly with respect to HLA phenotype or selected for the expression of one HLA allele without considering an influence of other HLA molecules. In addition, little information is available on the influence of HLA makeup on the overall CTL response against influenza viruses. Here, the influenza A virus-specific CTL response was investigated in groups of HLA-A and -B identical individuals. Between groups the individuals shared two or three of the four HLA-A and -B alleles. After in vitro stimulation of PBMC with influenza virus, the highest CTL activity was found in HLA-A2(+) donors. A similar pattern was observed for the precursor frequency of virus-specific CTL (CTLp) ex vivo, with a higher CTLp frequency in HLA-A2-positive donors than in HLA-A2-negative donors, which were unable to recognize the immunodominant M1(58-66) epitope. In addition, CTL activity and frequency of CTLp for the individual influenza virus epitopes were determined. The frequency of CTLp specific for the HLA-B8-restricted epitope NP(380-388) was threefold lower in HLA-B27-positive donors than in HLA-B27-negative donors. In addition, the frequency of CTLp specific for the HLA-A1-restricted epitope NP(44-52) was threefold higher in HLA-A1-, -A2-, -B8-, and -B35-positive donors than in other donors, which was confirmed by measuring the CTL activity in vitro. These findings indicate that the epitope specificity of the CTL response is related to the phenotype of the other HLA molecules. Furthermore, the magnitude of the influenza virus-specific CTL response seems dependent on the HLA-A and -B phenotypes.

摘要

已证明人类细胞毒性T淋巴细胞(CTL)针对甲型流感病毒的反应库针对多个表位,其中对HLA - A2限制性M1(58 - 66)表位有主要反应。然而,这些研究是针对HLA表型随机选择的个体的外周血单核细胞(PBMC)进行的,或者是选择表达一个HLA等位基因的个体进行的,而没有考虑其他HLA分子的影响。此外,关于HLA组成对针对流感病毒的总体CTL反应的影响,几乎没有可用信息。在此,对HLA - A和 - B相同的个体组进行了甲型流感病毒特异性CTL反应的研究。组内个体共享四个HLA - A和 - B等位基因中的两个或三个。用流感病毒体外刺激PBMC后,在HLA - A2(+)供体中发现了最高的CTL活性。在体外,针对病毒特异性CTL(CTLp)的前体频率也观察到类似模式,HLA - A2阳性供体中的CTLp频率高于HLA - A2阴性供体,后者无法识别免疫显性M1(58 - 66)表位。此外,还确定了个体流感病毒表位的CTL活性和CTLp频率。针对HLA - B8限制性表位NP(380 - 388)的CTLp频率在HLA - B27阳性供体中比在HLA - B27阴性供体中低三倍。此外,针对HLA - A1限制性表位NP(44 - 52)的CTLp频率在HLA - A1、 - A2、 - B8和 - B35阳性供体中比在其他供体中高三倍,这通过体外测量CTL活性得到证实。这些发现表明CTL反应的表位特异性与其他HLA分子的表型有关。此外,甲型流感病毒特异性CTL反应的强度似乎取决于HLA - A和 - B表型。

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