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人类自身免疫性疾病是特定抗原驱动的T细胞疾病:抗原的鉴定。

Human autoimmune diseases are specific antigen-driven T-cell diseases: identification of the antigens.

作者信息

Platsoucas Chris D, Oleszak Emilia L

机构信息

Department of Microbiology and Immunology, Temple University School of Medicine, 3400 North Broad Street, Philadelphia, PA 19140, USA.

出版信息

Immunol Res. 2007;38(1-3):359-72. doi: 10.1007/s12026-007-0044-9.

Abstract

We are investigating the hypothesis that most human autoimmune diseases are specific antigen-driven T-cell diseases. T-cell clones responding to specific antigenic epitopes are responsible for the initiation and/or the propagation of these diseases. Similarly, specific antigen-driven T-cell responses are responsible for the rejection of organ allografts and the immune response to tumors. Activated T cells provide the "engine" for the chronic inflammation that is associated with autoimmune diseases, organ graft rejection and tumor immunity. The best way to identify whether specific antigen-driven T cell responses are involved in the initiation and/or propagation of these disorders is to investigate whether T cells that infiltrate relevant tissues from these diseases contain monoclonal or oligoclonal, that is to say clonally expanded, populations of T cells. Identification of the T-cell antigen receptor (TCR) transcripts employed by the clonally expanded T cells in these patients permits the identification of the specific antigens that elicit these T-cell responses. These antigens may be responsible for the pathogenesis of these diseases. We will summarize here certain of our findings in this area of research.

摘要

我们正在研究这样一个假说

大多数人类自身免疫性疾病是特定抗原驱动的T细胞疾病。对特定抗原表位作出反应的T细胞克隆负责这些疾病的起始和/或传播。同样,特定抗原驱动的T细胞反应也负责器官异体移植的排斥反应以及对肿瘤的免疫反应。活化的T细胞为与自身免疫性疾病、器官移植排斥反应和肿瘤免疫相关的慢性炎症提供了“动力”。确定特定抗原驱动的T细胞反应是否参与这些疾病的起始和/或传播的最佳方法,是研究从这些疾病的相关组织中浸润的T细胞是否包含单克隆或寡克隆(即克隆性扩增)的T细胞群体。鉴定这些患者中克隆性扩增的T细胞所使用的T细胞抗原受体(TCR)转录本,能够确定引发这些T细胞反应的特定抗原。这些抗原可能是这些疾病发病机制的原因。我们将在此总结我们在这一研究领域的某些发现。

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