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人类皮肤被能够独立于脂质识别 CD1a 的 T 细胞定植。

Human skin is colonized by T cells that recognize CD1a independently of lipid.

机构信息

Graduate Program in Immunology, Harvard Medical School, Boston, Massachusetts, USA.

Division of Rheumatology, Inflammation and Immunity, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, USA.

出版信息

J Clin Invest. 2021 Jan 4;131(1). doi: 10.1172/JCI140706.

Abstract

CD1a-autoreactive T cells contribute to skin disease, but the identity of immunodominant self-lipid antigens and their mode of recognition are not yet solved. In most models, MHC and CD1 proteins serve as display platforms for smaller antigens. Here, we showed that CD1a tetramers without added antigen stained large T cell pools in every subject tested, accounting for approximately 1% of skin T cells. The mechanism of tetramer binding to T cells did not require any defined antigen. Binding occurred with approximately 100 lipid ligands carried by CD1a proteins, but could be tuned upward or downward with certain natural self-lipids. TCR recognition mapped to the outer A' roof of CD1a at sites remote from the antigen exit portal, explaining how TCRs can bind CD1a rather than carried lipids. Thus, a major antigenic target of CD1a T cell autoreactivity in vivo is CD1a itself. Based on their high frequency and prevalence among donors, we conclude that CD1a-specific, lipid-independent T cells are a normal component of the human skin T cell repertoire. Bypassing the need to select antigens and effector molecules, CD1a tetramers represent a simple method to track such CD1a-specific T cells from tissues and in any clinical disease.

摘要

CD1a 自身反应性 T 细胞可导致皮肤疾病,但目前仍未明确免疫优势自身脂质抗原的身份及其识别方式。在大多数模型中,MHC 和 CD1 蛋白充当较小抗原的展示平台。在此,我们发现,未添加抗原的 CD1a 四聚体可染色每个测试对象的大型 T 细胞池,约占皮肤 T 细胞的 1%。四聚体与 T 细胞结合的机制不需要任何特定的抗原。结合发生在大约 100 种由 CD1a 蛋白携带的脂质配体上,但某些天然自身脂质可以将其上调或下调。TCR 识别映射到 CD1a 的外 A' 穹顶,位于抗原出口门远侧的部位,这解释了 TCR 如何结合 CD1a 而不是携带的脂质。因此,CD1a 自身反应性 T 细胞在体内的一个主要抗原靶标是 CD1a 自身。基于供体中的高频率和普遍性,我们得出结论,CD1a 特异性、脂质非依赖性 T 细胞是人类皮肤 T 细胞库的正常组成部分。CD1a 四聚体绕过了选择抗原和效应分子的需要,代表了一种从组织和任何临床疾病中追踪此类 CD1a 特异性 T 细胞的简单方法。

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