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迟发性轴性脊柱关节炎:来自Reuma-check队列的数据。

Late-onset axial spondyloarthritis: data from Reuma-check cohort.

作者信息

Garcia-Salinas Rodrigo, Reyes-Jara Gisel, Almada Felicia, Ruta Santiago, Ramiro Sofia

机构信息

Rheumatology Unit, Hospital Italiano de La Plata - Universidad Nacional de La Plata, 51 Street, 1725, 1900, La Plata, Buenos Aires Province, Argentina.

Leiden University Medical Center, Leiden and Zuyderland Medical Center, Heerlen, The Netherlands.

出版信息

Clin Rheumatol. 2025 Feb;44(2):701-706. doi: 10.1007/s10067-024-07299-3. Epub 2024 Dec 30.

Abstract

OBJECTIVES

To estimate the prevalence of late-onset axial spondyloarthritis (lo-axSpA) and to identify clinical, laboratory, and imaging features associated with this phenotype.

METHODS

This single-center, observational study included patients diagnosed with axSpA from the "Reuma-check" SpA program. Patients with a symptom onset ≥ 45 years were classified as lo-axSpA, as opposed to early-onset axSpA (eo-axSpA, onset < 45 years). The prevalence of lo-axSpA was calculated, and lo-axSpA and eo-axSpA were compared in terms of clinical, laboratory and imaging characteristics. Factors associated with lo-axSpA were analyzed with univariable followed by multivariable logistic regression.

RESULTS

A total of 126 patients were included, 35 (28%) were lo-axSpA. Comparing lo-axSpA vs. eo-axSpA, significant differences were observed: higher female prevalence in lo-axSpA vs. eo-axSpA (51% vs. 29%), lower NSAID response (52% vs. 73%), increased skin psoriasis prevalence (42% vs. 17%,), and shorter diagnosis delay (40 vs. 93 months). In the multivariable analysis, male sex and diagnosis delay were independently and inversely associated with lo-axSpA (OR 0.2, 95% CI 0.06-0.8 and OR 0.9, 95% CI 0.96-0.99, respectively), while psoriasis was associated with a higher odds for lo-axSpA (OR 4.8, 95% CI 1.1-29).

CONCLUSION

lo-axSpA was present in more than a quarter of the patients. Although recall bias in the symptom duration cannot be excluded, the presentation with lo-axSpA seems to be associated with distinct features, being more frequent in females and more associated with psoriasis and with a shorter diagnostic delay. Key Points • Late-onset axSpA (≥ 45Y) is observed in 28% in our cohort, a higher frequency than previously reported. • Female sex and psoriasis are associated with a higher likelihood for late-onset axSpA.

摘要

目的

评估晚发型中轴型脊柱关节炎(lo-axSpA)的患病率,并确定与该表型相关的临床、实验室和影像学特征。

方法

这项单中心观察性研究纳入了“Reuma-check”脊柱关节炎项目中诊断为axSpA的患者。症状发作年龄≥45岁的患者被分类为lo-axSpA,与之相对的是早发型axSpA(eo-axSpA,发作年龄<45岁)。计算lo-axSpA的患病率,并比较lo-axSpA和eo-axSpA在临床、实验室和影像学特征方面的差异。采用单变量分析,随后进行多变量逻辑回归分析与lo-axSpA相关的因素。

结果

共纳入126例患者,其中35例(28%)为lo-axSpA。比较lo-axSpA和eo-axSpA,观察到显著差异:lo-axSpA中女性患病率高于eo-axSpA(51%对29%),非甾体抗炎药反应较低(52%对73%),皮肤银屑病患病率增加(42%对17%),诊断延迟时间较短(40个月对93个月)。在多变量分析中,男性和诊断延迟与lo-axSpA独立且呈负相关(比值比分别为0.2,95%置信区间0.06 - 0.8和0.9,95%置信区间0.96 - 0.99),而银屑病与lo-axSpA的较高患病几率相关(比值比4.8,95%置信区间1.1 - 29)。

结论

超过四分之一的患者存在lo-axSpA。尽管不能排除症状持续时间的回忆偏倚,但lo-axSpA的表现似乎与独特特征相关,在女性中更常见,且与银屑病关系更密切,诊断延迟更短。要点•在我们的队列中,28%观察到晚发型axSpA(≥45岁),频率高于先前报道。•女性和银屑病与晚发型axSpA的较高可能性相关。

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