主要组织相容性复合体(MHC)与类风湿关节炎的关联。类风湿关节炎(RA)与人类白细胞抗原-DR4(HLA-DR4)的关联: repertoire选择的作用 。 (注:“repertoire”此处可能专业术语,在医学免疫等领域有特定含义,比如免疫细胞受体库等,但仅按要求翻译,未详细解释 )
Association of MHC and rheumatoid arthritis. Association of RA with HLA-DR4: the role of repertoire selection.
作者信息
Roudier J
机构信息
Laboratoire d'Immunorhumatologie, INSERM EPI9940, Faculté de Médecine, Marseille, France.
出版信息
Arthritis Res. 2000;2(3):217-20. doi: 10.1186/ar91. Epub 2000 Apr 12.
Abstract
Most patients with rheumatoid arthritis (RA) express HLA-DR4, HLA-DR1 or HLA-DR10. These alleles share a common amino acid motif in their third hypervariable regions: the shared epitope. In normals and patients with RA, HLA-DR genes exert a major influence on the CD4 alpha beta T-cell repertoire, as shown by studies of AV and BV gene usage and by BV BJ gene usage by peripheral blood CD4 alpha beta T-cells. However, the rheumatoid T-cell repertoire is not entirely under HLA-DR influence, as demonstrated by discrepancies in VB JB gene usage between identical twins discordant for RA and by contraction of the CD4 alpha beta T-cell repertoire in RA patients. Shared epitope positive HLA-DR alleles may shape the T-cell repertoire by presenting self peptides to CD4 T cells in the thymus. Peptides processed from HLA-DR molecules and encompassing the shared epitope may also be presented by HLA-DQ and select CD4 alpha beta T cells in the thymus. Thus, shared epitope-positive alleles impose a frame on the T-cell repertoire. This predisposing frame is further modified (by unknown factors) to obtain the contracted rheumatoid repertoire.
摘要
大多数类风湿关节炎(RA)患者表达HLA - DR4、HLA - DR1或HLA - DR10。这些等位基因在其第三个高变区共享一个共同的氨基酸基序:共享表位。在正常人和RA患者中,HLA - DR基因对CD4αβT细胞库有主要影响,这已通过对AV和BV基因使用情况以及外周血CD4αβT细胞的BV BJ基因使用情况的研究得到证实。然而,类风湿T细胞库并不完全受HLA - DR影响,这已通过患RA的同卵双胞胎之间VB JB基因使用情况的差异以及RA患者中CD4αβT细胞库的收缩得到证明。共享表位阳性的HLA - DR等位基因可能通过在胸腺中向CD4 T细胞呈递自身肽来塑造T细胞库。从HLA - DR分子加工而来且包含共享表位的肽也可能由HLA - DQ呈递,并在胸腺中选择CD4αβT细胞。因此,共享表位阳性等位基因给T细胞库设定了一个框架。这个易患框架会(通过未知因素)进一步改变,以形成收缩的类风湿细胞库。
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