Quaratino S, Feldmann M, Dayan C M, Acuto O, Londei M
Mathilda & Terence Kennedy Institute of Rheumatology, Sunley Division, London, United Kingdom.
J Exp Med. 1996 Feb 1;183(2):349-58. doi: 10.1084/jem.183.2.349.
Recognition of self-antigens by T lymphocytes is a central event in autoimmunity. Understanding of the molecular interactions between T cell receptors (TCR) and self-epitopes may explain how T cells escape thymic education and initiate an autoimmune reaction. We have studied five human in vivo activated T cell clones specific for the region 535-551 of human thyroid peroxidase (TPO) established from a Graves' patient. Three clones (37, 72, and 73) expressed identical TCR beta and alpha chains rearranging V beta 1.1 and V alpha 15.1, and were considered sister clones. Clone 43 differed from clone 37 and its sisters in the J alpha region only. Clone NP-7 expressed V beta 6.5 but rearranged two in-frame TCR alpha chain, both using the V alpha 22.1 segment. Fine epitope mapping using nested peptides showed that clones using identical TCR beta chains, identical V alpha, but a different J alpha recognized distinct, nonoverlapping epitopes in the TPO 535-551 region. This finding shows that a different J alpha region alone leads to a heterogeneous pattern of recognition. This indicates that the "restricted" TCR V region usage sometimes found in autoimmune diseases may not always correspond to identical epitope recognition. To confirm that clones 37 (and its sisters) and 43 recognize different epitopes, the T cell clones were stimulated with a TPO-transfected autologous Epstein-Barr virus (EBV) cell line (TPO-EBV) that presents TPO epitopes afer endogenous processing. Only clone 37 and its sisters recognizes the TPO-EBV cell line, suggesting that the epitope recognized by clone 43 is not presented upon endogenous processing. We have shown that thyroid epithelial cells (TEC), the only cells that produce TPO, express HLA class II molecules in Graves' disease and can act as an antigen-presenting cells, presenting TPO after endogenous processing to autoantigen-reactive T cell clones. We tested, therefore, whether autologous TEC induced the same pattern of stimulation as TPO-EBV; T cell clone 37 recognizes the TEC, whereas it is stimulated poorly by the TPO loaded to autologous peripheral blood mononuclear cells (PBMC). Clone 43, which fails to recognize the TPO-EBV, also fails to recognize the TEC, but is activated by exogenous TPO presented by autologous PBMC. These results show that exogenous versus endogenous processing in vivo generates a different TPO epitope repertoire, producing a "cryptic" epitope (epitope not always available for recognition). Our findings define a route by which human self-reactive T cells may escape thymic selection and become activated in vivo, thus possibly leading to autoimmunity.
T淋巴细胞对自身抗原的识别是自身免疫中的核心事件。了解T细胞受体(TCR)与自身表位之间的分子相互作用,或许可以解释T细胞如何逃避胸腺教育并引发自身免疫反应。我们研究了从一名格雷夫斯病患者体内建立的五个对人甲状腺过氧化物酶(TPO)535 - 551区域具有特异性的体内活化人T细胞克隆。三个克隆(37、72和73)表达相同的TCRβ和α链,重排的是Vβ1.1和Vα15.1,被视为姐妹克隆。克隆43仅在Jα区域与克隆37及其姐妹克隆不同。克隆NP - 7表达Vβ6.5,但重排了两条符合读框的TCRα链,二者均使用Vα22.1区段。使用嵌套肽进行精细表位图谱分析表明,使用相同TCRβ链、相同Vα但不同Jα的克隆在TPO 535 - 551区域识别不同的、不重叠的表位。这一发现表明,仅一个不同的Jα区域就会导致识别模式的异质性。这表明在自身免疫疾病中有时发现的“受限”TCR V区域使用情况可能并不总是对应相同的表位识别。为了证实克隆37(及其姐妹克隆)和43识别不同的表位,用一种经TPO转染的自体爱泼斯坦 - 巴尔病毒(EBV)细胞系(TPO - EBV)刺激T细胞克隆,该细胞系在内源加工后呈递TPO表位。只有克隆37及其姐妹克隆识别TPO - EBV细胞系,这表明克隆43识别的表位在内源加工后不会被呈递。我们已经表明,甲状腺上皮细胞(TEC)是唯一产生TPO的细胞,在格雷夫斯病中表达HLA II类分子,并且可以作为抗原呈递细胞,在内源加工后将TPO呈递给自身抗原反应性T细胞克隆。因此,我们测试了自体TEC是否能诱导与TPO - EBV相同的刺激模式;T细胞克隆37识别TEC,而负载了TPO的自体外周血单核细胞(PBMC)对其刺激较弱。克隆43不能识别TPO - EBV,也不能识别TEC,但能被自体PBMC呈递的外源性TPO激活。这些结果表明,体内的外源性加工与内源性加工产生了不同的TPO表位库,产生了一个“隐蔽”表位(并非总是可用于识别的表位)。我们的发现确定了一条人类自身反应性T细胞可能逃避胸腺选择并在体内被激活的途径,从而可能导致自身免疫。
