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胰高血糖素样肽-1受体激动剂与银屑病患者死亡率、心血管及精神疾病风险降低:一项大规模队列研究

GLP-1RA and reduced mortality, cardiovascular and psychiatric risks in psoriasis: a large-scale cohort study.

作者信息

Olbrich Henning, Kridin Khalaf, Zirpel Henner, Hernandez Gema, Sadik Christian D, Gaffal Evelyn, Thaçi Diamant, Ludwig Ralf J

机构信息

Department of Dermatology, Allergy, and Venerology, University of Lübeck, Lübeck, Germany.

Unit of Dermatology and Skin Research Laboratory, Galilee Medical Center, Nahariya, Israel.

出版信息

Br J Dermatol. 2025 Sep 3. doi: 10.1093/bjd/ljaf346.

Abstract

BACKGROUND

Psoriasis is associated with a significant comorbidity burden, especially cardiovascular and metabolic complications. Glucagon-like peptide-1 receptor agonists (GLP-1RA), such as semaglutide, used to treat obesity and diabetes, could potentially reduce comorbidity in patients with psoriasis.

OBJECTIVE

To investigate all-cause mortality, cardiovascular, inflammatory, psychiatric outcomes, and adverse events in psoriasis patients treated with GLP-1RA.

METHODS

This retrospective population-based cohort study utilized real-world data from the US TriNetX database. Patients with psoriasis who were treated for diabetes or obesity with GLP-1RA during the full follow-up period of 2 years were compared with those treated with other systemic anti-diabetic or obesity drugs. After 1:1 propensity-score matching for relevant risk factors, 3,048 participants were included in each cohort. The primary outcomes included the risk of cardiometabolic, psychiatric, and autoimmune sequelae of psoriasis, as well as all-cause mortality and potential adverse drug events. The analysis was repeated using cohorts without psoriasis and results were further validated through two sensitivity analyses involving (i) later follow-up periods, or (ii) exclusion of patients with pustular psoriasis.

RESULTS

In the matched cohorts of 3,048 patients with psoriasis treated with GLP-1RA (60.37% females, mean age 56.94 years, standard deviation [SD] 12.02 years) versus other antidiabetic and obesity drugs (61.91% females, mean age 56.42 years, SD 14.16 years), GLP-1RA treatment was associated with significantly decreased all-cause mortality (hazard ratio [HR] 0.219, 95% confidence interval [CI] 0.123-0.391, p<0.0001) and reduced risk for major adverse cardiac events (MACE, HR 0.561, 95% CI 0.442-0.714, p<0.0001). Additionally, lower risks for alcohol (HR 0.346, CI 0.174-0.685, p=0.009) and substance abuse (HR 0.510, CI 0.350-0.743, p=0.002) were observed. Typical adverse drug events were not more frequent in the GLP-1RA cohort. The risk reductions were more pronounced in the cohorts with psoriasis compared to persons with obesity or diabetes without psoriasis. Findings were consistent across all sensitivity analyses.

CONCLUSIONS

GLP-1RA treatment was safe and associated with reduced risks of cardiovascular and psychiatric comorbidities, as well as lower mortality in patients with psoriasis, with risk reductions markedly higher than in cohorts without psoriasis. Physicians should consider this drug class for patients with psoriasis and comorbid obesity or diabetes.

摘要

背景

银屑病与显著的合并症负担相关,尤其是心血管和代谢并发症。胰高血糖素样肽-1受体激动剂(GLP-1RA),如司美格鲁肽,用于治疗肥胖和糖尿病,可能会降低银屑病患者的合并症。

目的

研究接受GLP-1RA治疗的银屑病患者的全因死亡率、心血管、炎症、精神方面的结局以及不良事件。

方法

这项基于人群的回顾性队列研究利用了来自美国TriNetX数据库的真实世界数据。将在2年的完整随访期内接受GLP-1RA治疗糖尿病或肥胖的银屑病患者与接受其他全身性抗糖尿病或肥胖药物治疗的患者进行比较。在对相关风险因素进行1:1倾向评分匹配后,每个队列纳入3048名参与者。主要结局包括银屑病的心脏代谢、精神和自身免疫后遗症风险,以及全因死亡率和潜在的药物不良事件。使用无银屑病的队列重复分析,并通过两项敏感性分析进一步验证结果,这两项分析涉及(i)更长的随访期,或(ii)排除脓疱型银屑病患者。

结果

在3048名接受GLP-1RA治疗的银屑病患者(60.37%为女性,平均年龄56.94岁,标准差[SD]12.02岁)与其他抗糖尿病和肥胖药物治疗患者(61.91%为女性,平均年龄56.42岁,SD 14.16岁)的匹配队列中,GLP-1RA治疗与全因死亡率显著降低(风险比[HR]0.219,95%置信区间[CI]0.123 - 0.391,p<0.0001)以及主要不良心脏事件(MACE)风险降低(HR 0.561,95% CI 0.442 - 0.714,p<0.0001)相关。此外,观察到酒精(HR 0.346,CI 0.174 - 0.685,p = 0.009)和药物滥用(HR 0.510,CI 0.350 - 0.743,p = 0.002)风险较低。GLP-1RA队列中典型的药物不良事件并不更频繁。与无银屑病的肥胖或糖尿病患者相比,银屑病队列中的风险降低更为明显。所有敏感性分析的结果均一致。

结论

GLP-1RA治疗是安全的,与银屑病患者心血管和精神合并症风险降低以及死亡率降低相关,风险降低明显高于无银屑病的队列。医生应为患有银屑病合并肥胖或糖尿病的患者考虑这类药物。

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