Rheumatology Department, Sainte Marguerite Hospital, Aix-Marseille University, APHM, Marseille, France.
Autoimmune Arthritis Laboratory, INSERM UMRs1097, Aix Marseille University, Marseille, France.
Front Immunol. 2022 Nov 30;13:1054539. doi: 10.3389/fimmu.2022.1054539. eCollection 2022.
Psoriatic arthritis (PsA) is a chronic inflammatory disease that frequently develops in patients with psoriasis (PsO) but can also occur spontaneously. As a result, PsA diagnosis and treatment is commonly delayed, or even missed outright due to the manifold of clinical presentations that patients often experience. This inevitably results in progressive articular damage to axial and peripheral joints and entheses. As such, patients with PsA frequently experience reduced expectancy and quality of life due to disability. More recently, research has aimed to improve PsA diagnosis and prognosis by identifying novel disease biomarkers.
Here, we conducted a systematic review of the published literature on candidate biomarkers for PsA diagnosis and prognosis in MEDLINE(Pubmed), EMBase and the Cochrane library with the goal to identify clinically applicable PsA biomarkers. Meta-analyses were performed when a diagnostic bone and cartilage turnover biomarker was reported in 2 or moredifferent cohorts of PsA and control.
We identified 1444 publications and 124 studies met eligibility criteria. We highlighted bone and cartilage turnover biomarkers, genetic markers, and autoantibodies used for diagnostic purposes of PsA, as well as acute phase reactant markers and bone and cartilage turnover biomarkers for activity or prognostic severity purposes. Serum cartilage oligometrix metalloproteinase levels were significantly increased in the PsA sera compared to Healthy Control (HC) with a standardized mean difference (SMD) of 2.305 (95%CI 0.795-3.816, p=0.003) and compared to osteoarthritis (OA) with a SMD of 0.783 (95%CI 0.015-1.551, p=0.046). The pooled serum MMP-3 levels were significantly higher in PsA patients than in PsO patients with a SMD of 0.419 (95%CI 0.119-0.719; p=0.006), but no significant difference was highlighted when PsA were compared to HC. While we did not identify any new genetic biomarkers that would be useful in the diagnosis of PsA, recent data with autoantibodies appear to be promising in diagnosis, but no replication studies have been published.
In summary, no specific diagnostic biomarkers for PsA were identified and further studies are needed to assess the performance of potential biomarkers that can distinguish PsA from OA and other chronic inflammatory diseases.
银屑病关节炎(PsA)是一种慢性炎症性疾病,常发生在银屑病(PsO)患者中,但也可自发发生。因此,由于患者常经历多种临床表现,PsA 的诊断和治疗通常会延迟,甚至完全错过。这不可避免地导致轴向和外周关节及附着点的进行性关节损伤。因此,由于残疾,患有 PsA 的患者通常预期寿命和生活质量降低。最近,研究旨在通过识别新的疾病生物标志物来改善 PsA 的诊断和预后。
在这里,我们在 MEDLINE(PubMed)、EMBase 和 Cochrane 图书馆中对发表的有关 PsA 诊断和预后候选生物标志物的文献进行了系统综述,目的是确定临床上可应用的 PsA 生物标志物。当报告了 2 个或更多不同的 PsA 队列和对照组的诊断性骨和软骨转换生物标志物时,我们进行了荟萃分析。
我们确定了 1444 篇出版物和 124 项符合入选标准的研究。我们强调了用于 PsA 诊断目的的骨和软骨转换生物标志物、遗传标志物和自身抗体,以及用于活动或预后严重程度目的的急性期反应物标志物和骨和软骨转换生物标志物。与健康对照(HC)相比,PsA 血清中的软骨寡聚基质蛋白水平显著升高,标准化均数差(SMD)为 2.305(95%CI 0.795-3.816,p=0.003),与骨关节炎(OA)相比,SMD 为 0.783(95%CI 0.015-1.551,p=0.046)。与 PsO 患者相比,PsA 患者的血清 MMP-3 水平显著升高,SMD 为 0.419(95%CI 0.119-0.719;p=0.006),但与 HC 相比,无显著差异。虽然我们没有发现任何新的遗传生物标志物对 PsA 的诊断有用,但最近的自身抗体数据似乎很有希望用于诊断,但尚未发表复制研究。
总之,未确定用于 PsA 的特定诊断生物标志物,需要进一步研究来评估可区分 PsA 与 OA 和其他慢性炎症性疾病的潜在生物标志物的性能。
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