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前沿:胸腺选择和自身反应性受参与T细胞活化的多种共受体调控。

Cutting edge: thymic selection and autoreactivity are regulated by multiple coreceptors involved in T cell activation.

作者信息

Page D M

机构信息

Department of Biology, Cancer Center, University of California at San Diego, La Jolla 92093, USA.

出版信息

J Immunol. 1999 Oct 1;163(7):3577-81.

Abstract

Immune responses are shaped by several processes that promote responses to pathogens and hinder responses to self. One mechanism that contributes to this polarization in response is negative selection, in which thymocytes that can respond to self-peptide/MHC complexes are deleted from the T cell repertoire. I found here that several coreceptors known to contribute to mature T cell activation also participate in negative selection. Interestingly, these molecules appeared to act in a cooperative fashion. Blocking the contribution of these molecules in fetal thymus organ culture not only prevented negative selection in the CD4+ lineage, but also induced the appearance of autoreactive thymocytes. This is the first demonstration that blocking coreceptor interactions during thymic development can produce autoreactive T cells. The contribution of negative selection to the mature T cell repertoire and to autoimmunity is discussed in light of these results.

摘要

免疫反应由多种促进对病原体反应并阻碍对自身反应的过程所塑造。促成这种反应极化的一种机制是阴性选择,即能对自身肽/MHC复合物产生反应的胸腺细胞从T细胞库中被清除。我在此发现,已知有助于成熟T细胞活化的几种共受体也参与阴性选择。有趣的是,这些分子似乎以协同方式发挥作用。在胎儿胸腺器官培养中阻断这些分子的作用不仅阻止了CD4+谱系中的阴性选择,还诱导了自身反应性胸腺细胞的出现。这是首次证明在胸腺发育过程中阻断共受体相互作用可产生自身反应性T细胞。根据这些结果讨论了阴性选择对成熟T细胞库和自身免疫的贡献。

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