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前沿:通过I型干扰素直接刺激B细胞和T细胞增强抗体反应

Cutting edge: enhancement of antibody responses through direct stimulation of B and T cells by type I IFN.

作者信息

Le Bon Agnes, Thompson Clare, Kamphuis Elisabeth, Durand Vanessa, Rossmann Cornelia, Kalinke Ulrich, Tough David F

机构信息

The Edward Jenner Institute for Vaccine Research, Compton, Newbury, Berkshire, UK.

出版信息

J Immunol. 2006 Feb 15;176(4):2074-8. doi: 10.4049/jimmunol.176.4.2074.

Abstract

Type I IFN (IFN-alphabeta) is induced rapidly by infection and plays a key role in innate antiviral defense. IFN-alphabeta also exerts stimulatory effects on the adaptive immune system and has been shown to enhance Ab and T cell responses. We have investigated the importance of B and T cells as direct targets of IFN-alphabeta during IFN-alpha-mediated augmentation of the Ab response against a soluble protein Ag. Strikingly, the ability of IFN-alpha to stimulate the Ab response and induce isotype switching was markedly reduced in mice in which B cells were selectively deficient for the IFN-alphabetaR. Moreover, IFN-alpha-mediated enhancement of the Ab response was also greatly impaired in mice in which T cells were selectively IFN-alphabetaR-deficient. These results indicate that IFN-alphabetaR signaling in both B and T cells plays an important role in the stimulation of Ab responses by IFN-alphabeta.

摘要

I型干扰素(IFN-αβ)在感染后迅速产生,在先天性抗病毒防御中起关键作用。IFN-αβ对适应性免疫系统也有刺激作用,并已被证明可增强抗体和T细胞反应。我们研究了在IFN-α介导的针对可溶性蛋白抗原的抗体反应增强过程中,B细胞和T细胞作为IFN-αβ直接靶点的重要性。令人惊讶的是,在B细胞选择性缺乏IFN-αβ受体的小鼠中,IFN-α刺激抗体反应和诱导同种型转换的能力明显降低。此外,在T细胞选择性缺乏IFN-αβ受体的小鼠中,IFN-α介导的抗体反应增强也受到极大损害。这些结果表明,B细胞和T细胞中的IFN-αβ受体信号传导在IFN-αβ刺激抗体反应中起重要作用。

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