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在系统性红斑狼疮轻度疾病活动中对炎症的更高遗传易感性。

Higher genetic susceptibility to inflammation in mild disease activity of systemic lupus erythematosus.

作者信息

Tsai Li-Jen, Hsiao Sheng-Hsiung, Tsai Jaw-Ji, Lin Ching-Yuang, Tsai Lih-Min, Lan Joung-Liang

机构信息

College of Engineering, National Taiwan University of Science and Technology, Taipei, 10672, Taiwan.

出版信息

Rheumatol Int. 2009 Jul;29(9):1001-11. doi: 10.1007/s00296-009-0900-0. Epub 2009 Apr 28.

Abstract

In order to test the hypothesis that stratification of Mexican Modification of the Systemic Lupus Erythematosus Disease Activity Index (MEX-SLEDAI) simplifies the genetic study of SLE, we evaluated the genetic susceptibility to inflammation and defects in clearance of immune complexes among SLE patients in Taiwan. SLE phenotypes were stratified according to the MEX-SLEDAI scores into two subgroups (<or=10 and >10), and then according to renal disorder and neurological disorder, aiming to minimize any loss of power associated with disease heterogeneity. Upon stratification, IL1-beta polymorphism and LTA were significantly associated with SLE within the MEX-SLEDAI <or=10 subgroup. When SLE patients were classified into two subgroups with or without renal disorder to stratify the genetic study, we could find that the stratification with renal disorder could partially confirm the hypothesis that stratification of MEX-SLEDAI score simplifies the genetic study of complex diseases such as SLE. So we concluded that in the mild disease state of SLE, stratification of disease phenotypes, especially IL1-beta and LTA, according to MEX-SLEDAI scores could reveal new associations between candidate genes and disease activity index of SLE.

摘要

为了验证墨西哥版系统性红斑狼疮疾病活动指数(MEX-SLEDAI)分层能够简化系统性红斑狼疮(SLE)基因研究这一假设,我们评估了台湾SLE患者的炎症遗传易感性以及免疫复合物清除缺陷情况。根据MEX-SLEDAI评分将SLE表型分为两个亚组(≤10和>10),然后再根据肾脏疾病和神经系统疾病进行分层,旨在尽量减少与疾病异质性相关的效能损失。分层后,在MEX-SLEDAI≤10亚组中,IL1-β多态性和LTA与SLE显著相关。当将SLE患者按有无肾脏疾病分为两个亚组以分层基因研究时,我们发现按肾脏疾病分层可部分证实MEX-SLEDAI评分分层能简化SLE等复杂疾病基因研究这一假设。因此我们得出结论,在SLE的轻度疾病状态下,根据MEX-SLEDAI评分对疾病表型进行分层,尤其是对IL1-β和LTA进行分层,能够揭示候选基因与SLE疾病活动指数之间的新关联。

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