Department of Epidemiology and Health Statistics, School of Public Health, Shandong First Medical University & Shandong Academy of Medical Sciences, Tai'an, China.
Department of Rheumatology and Immunology, Liaocheng People's Hospital, Liao'cheng, China.
Front Immunol. 2021 Jun 29;12:682400. doi: 10.3389/fimmu.2021.682400. eCollection 2021.
Systemic lupus erythematosus (SLE) affects many organs and systems of the human organism, at present, its specific pathogenesis is not completely clear, but inflammation is considered to be an important factor involved in the pathogenesis and progression of SLE. Gamma-glutamyl transpeptidase (GGT) and total bilirubin (TBIL) have different effects on inflammation: GGT has pro-inflammatory effects, on the contrary, TBIL has anti-inflammatory effects. Study has found that GGT and TBIL play opposite roles in metabolic diseases. However, the roles of them in SLE are unknown. Meanwhile, the relationship between GGT and SLE also remains unexplored.
We recruited 341 SLE patients and 332 healthy individuals in Liaocheng People's Hospital from August 2018 to May 2019. We diagnosed SLE using 2019 revised American College of Rheumatology (ACR) SLE criteria, and modeled the study outcomes using logistic regression to explore the respective relationship between GGT, TBIL and SLE. We also analyzed the interaction of GGT and TBIL in the progression of SLE.
We found that the levels of CRP, IL-6 and TNF-α in the aggravated group were significantly higher than those in the unaggravated group, the levels of C3 and C4 in the aggravated group were significantly lower than those in the unaggravated group. According to Spearman correlation analysis, GGT is proportional to CRP (r=0.417) and IL-6 (r=0.412), inversely proportional to C3 (r=-0.177) and C4 (r=0.-132). TBIL was inversely proportional to CRP (r=-0.328) and TNF(r=-0.360), and positively proportional to C3 (r=0.174) and C4 (r=0.172). In the fully adjusted model, compared to the lowest quartile, the highest quartile of GGT exhibited a positive association with the risk of SLE aggravation (OR=2.99, 95% CI: 1.42-6.31, <0.001). At the same time, compared to the highest quartile, the quartile lowest of TBIL exhibited a positive association with the risk of SLE aggravation (OR=2.66, 95% CI: 1.27-5.59, <0.001) in the fully adjusted model. Through interaction analysis, we found that women with high GGT levels had an increased risk of SLE aggravation when they had a low level of TBIL (OR=3.68, 95% CI: 1.51-9.01, for women with Q1 TBIL and Q4 GGT compared to women with Q2-Q4 TBIL and Q1-Q3 GGT, for interaction <0.001), the combined AUC value (AUC=0.711) of high GGT level and TBIL were higher than their respective values (AUC=0.612, AUC=0.614).
We found that the effects of GGT and TBIL in the progression of SLE are opposite. High GGT level might be a risk factor for SLE aggravation, as GGT levels increased, so did the risk of SLE aggravation. At the same time, we found that low TBIL level might be a risk factor for SLE aggravation. Moreover, high GGT level and low TBIL level had a subadditive effect on the increased risk of SLE aggravation.
系统性红斑狼疮(SLE)影响人体的许多器官和系统,目前其具体发病机制尚不完全清楚,但炎症被认为是参与 SLE 发病和进展的重要因素。γ-谷氨酰转肽酶(GGT)和总胆红素(TBIL)对炎症有不同的影响:GGT 具有促炎作用,相反,TBIL 具有抗炎作用。研究发现 GGT 和 TBIL 在代谢性疾病中发挥相反的作用。然而,它们在 SLE 中的作用尚不清楚。同时,GGT 与 SLE 之间的关系也尚未得到探索。
我们在 2018 年 8 月至 2019 年 5 月期间在聊城市人民医院招募了 341 名 SLE 患者和 332 名健康对照者。我们使用 2019 年修订的美国风湿病学会(ACR)SLE 标准诊断 SLE,并使用逻辑回归模型来探索 GGT、TBIL 与 SLE 之间的各自关系。我们还分析了 GGT 和 TBIL 在 SLE 进展中的相互作用。
我们发现,加重组的 CRP、IL-6 和 TNF-α 水平明显高于未加重组,加重组的 C3 和 C4 水平明显低于未加重组。根据 Spearman 相关分析,GGT 与 CRP(r=0.417)和 IL-6(r=0.412)呈比例关系,与 C3(r=-0.177)和 C4(r=-0.132)呈反比关系。TBIL 与 CRP(r=-0.328)和 TNF(r=-0.360)呈反比关系,与 C3(r=0.174)和 C4(r=0.172)呈正比关系。在完全调整的模型中,与最低四分位数相比,GGT 的最高四分位数与 SLE 加重的风险呈正相关(OR=2.99,95%CI:1.42-6.31,<0.001)。同时,与最高四分位数相比,TBIL 的最低四分位数与 SLE 加重的风险呈正相关(OR=2.66,95%CI:1.27-5.59,<0.001)在完全调整的模型中。通过交互分析,我们发现,当女性 GGT 水平较高且 TBIL 水平较低时,她们患 SLE 加重的风险会增加(OR=3.68,95%CI:1.51-9.01,与 Q1 TBIL 和 Q4 GGT 相比,与 Q2-Q4 TBIL 和 Q1-Q3 GGT 相比,交互作用<0.001),GGT 水平高和 TBIL 低的联合 AUC 值(AUC=0.711)高于各自的 AUC 值(AUC=0.612,AUC=0.614)。
我们发现 GGT 和 TBIL 在 SLE 进展中的作用相反。高 GGT 水平可能是 SLE 加重的危险因素,随着 GGT 水平的升高,SLE 加重的风险也随之增加。同时,我们发现低 TBIL 水平可能是 SLE 加重的危险因素。此外,GGT 水平高和 TBIL 水平低对 SLE 加重风险的增加有亚加性效应。
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