Systemic evaluation of the relationship between psoriasis, psoriatic arthritis and osteoporosis: observational and Mendelian randomisation study

医学 银屑病 银屑病性关节炎 内科学 骨质疏松症 骨量减少 混淆 关节炎 皮肤病科 观察研究 物理疗法 骨矿物
作者
Jiangwei Xia,Songqiang Xie,Ke-Qi Liu,Lin Xu,Pianpian Zhao,Si-Rui Gai,Peng-Lin Guan,Jinqiu Zhao,Yanping Zhu,Lam C. Tsoi,Philip E. Stuart,Rajan P. Nair,Han-Qi Yang,Yuting Liao,Kaijing Mao,Mo-Chang Qiu,Zhimin Ying,Bin Hu,Zhihua Yang,Wenming Bai,Xiaowei Zhu,Peikuan Cong,James T. Elder,Zhaoming Ye,Bin Wang,Hou-Feng Zheng
出处
期刊:Annals of the Rheumatic Diseases [BMJ]
卷期号:79 (11): 1460-1467 被引量:39
标识
DOI:10.1136/annrheumdis-2020-217892
摘要

With 432 513 samples from UK Biobank dataset, multivariable linear/logistic regression were used to estimate the relationship between psoriasis/psoriatic arthritis (PsA) and estimated bone mineral density (eBMD)/osteoporosis, controlling for potential confounders. Here, confounders were set in three ways: model0 (including age, height, weight, smoking and drinking), model1 (model0 +regular physical activity) and model2 (model1 +medication treatments). The eBMD was derived from heel ultrasound measurement. And 4904 patients with psoriasis and 847 patients with PsA were included in final analysis. Mendelian randomisation (MR) approach was used to evaluate the causal effect between them.Lower eBMD were observed in patients with PsA than in controls in both model0 (β-coefficient=-0.014, p=0.0006) and model1 (β-coefficient=-0.013, p=0.002); however, the association disappeared when conditioning on treatment with methotrexate or ciclosporin (model2) (β-coefficient=-0.005, p=0.28), mediation analysis showed that 63% of the intermediary effect on eBMD was mediated by medication treatment (p<2E-16). Patients with psoriasis without arthritis showed no difference of eBMD compared with controls. Similarly, the significance of higher risk of osteopenia in patients with PsA (OR=1.27, p=0.002 in model0) could be eliminated by conditioning on medication treatment (p=0.244 in model2). Psoriasis without arthritis was not related to osteopenia and osteoporosis. The weighted Genetic Risk Score analysis found that genetically determined psoriasis/PsA were not associated with eBMD (p=0.24 and p=0.88). Finally, MR analysis showed that psoriasis/PsA had no causal effect on eBMD, osteoporosis and fracture.The effect of PsA on osteoporosis was secondary (eg, medication) but not causal. Under this hypothesis, psoriasis without arthritis was not a risk factor for osteoporosis.
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