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HLA-DRB1 位置 11 上缬氨酸和亮氨酸与类风湿关节炎影像学进展相关,与共享表位等位基因相关,但与抗瓜氨酸化蛋白抗体无关。

Association of valine and leucine at HLA-DRB1 position 11 with radiographic progression in rheumatoid arthritis, independent of the shared epitope alleles but not independent of anti-citrullinated protein antibodies.

机构信息

Leiden University Medical Center, Leiden, The Netherlands.

出版信息

Arthritis Rheumatol. 2015 Apr;67(4):877-86. doi: 10.1002/art.39018.

Abstract

OBJECTIVE

For decades it has been known that the HLA-DRB1 shared epitope (SE) alleles are associated with an increased risk of development and progression of rheumatoid arthritis (RA). Recently, the following variations in the peptide-binding grooves of HLA molecules that predispose to RA development have been identified: Val and Leu at HLA-DRB1 position 11, Asp at HLA-B position 9, and Phe at HLA-DPB1 position 9. This study was undertaken to investigate whether these variants are also associated with radiographic progression in RA, independent of SE and anti-citrullinated protein antibody (ACPA) status.

METHODS

A total of 4,911 radiograph sets from 1,878 RA patients included in the Leiden Early Arthritis Clinic (The Netherlands), Umeå (Sweden), Hospital Clinico San Carlos-Rheumatoid Arthritis (Spain), and National Data Bank for Rheumatic Diseases (US) cohorts were studied. HLA was imputed using single-nucleotide polymorphism data from an Immunochip, and the amino acids listed above were tested in relation to radiographic progression per cohort using an additive model. Results from the 4 cohorts were combined in inverse-variance weighted meta-analyses using a fixed-effects model. Analyses were conditioned on SE and ACPA status.

RESULTS

Val and Leu at HLA-DRB1 position 11 were associated with more radiographic progression (meta-analysis P = 5.11 × 10(-7)); this effect was independent of SE status (meta-analysis P = 0.022) but not independent of ACPA status. Phe at HLA-DPB1 position 9 was associated with more severe radiographic progression (meta-analysis P = 0.024), though not independent of SE status. Asp at HLA-B position 9 was not associated with radiographic progression.

CONCLUSION

Val and Leu at HLA-DRB1 position 11 conferred a risk of a higher rate of radiographic progression independent of SE status but not independent of ACPA status. These findings support the relevance of these amino acids at position 11.

摘要

目的

几十年来,人们一直知道 HLA-DRB1 共享表位(SE)等位基因与类风湿关节炎(RA)的发展和进展风险增加有关。最近,已经确定了以下导致 RA 发展的 HLA 分子肽结合槽中的变异:HLA-DRB1 位置 11 的 Val 和 Leu、HLA-B 位置 9 的 Asp 和 HLA-DPB1 位置 9 的 Phe。本研究旨在调查这些变体是否也与 RA 的放射学进展有关,而与 SE 和抗瓜氨酸蛋白抗体(ACPA)状态无关。

方法

研究了莱顿早期关节炎诊所(荷兰)、于默奥(瑞典)、圣卡洛斯临床医院-类风湿关节炎(西班牙)和国家风湿病数据银行(美国)队列中纳入的 1878 例 RA 患者的 4911 套放射图像。使用免疫芯片中的单核苷酸多态性数据对 HLA 进行推断,并使用加性模型根据每个队列的放射学进展对上述氨基酸进行测试。使用固定效应模型对 4 个队列的结果进行逆方差加权荟萃分析。分析条件为 SE 和 ACPA 状态。

结果

HLA-DRB1 位置 11 的 Val 和 Leu 与更多的放射学进展相关(荟萃分析 P = 5.11×10(-7));这种影响独立于 SE 状态(荟萃分析 P = 0.022),但不独立于 ACPA 状态。HLA-DPB1 位置 9 的 Phe 与更严重的放射学进展相关(荟萃分析 P = 0.024),尽管不独立于 SE 状态。HLA-B 位置 9 的 Asp 与放射学进展无关。

结论

HLA-DRB1 位置 11 的 Val 和 Leu 独立于 SE 状态但不独立于 ACPA 状态赋予了更高放射学进展率的风险。这些发现支持位置 11 上这些氨基酸的相关性。

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