Marklund Josefin, Hanna Balsam, Jin Tao, Pullerits Rille
Department of Rheumatology, Sahlgrenska University Hospital, Gothenburg, Sweden.
Department of Rheumatology and Inflammation Research, Institute of Medicine, Sahlgrenska Academy at University of Gothenburg, Gothenburg, Sweden.
Front Med (Lausanne). 2024 Mar 28;11:1340310. doi: 10.3389/fmed.2024.1340310. eCollection 2024.
Idiopathic inflammatory myopathies (IIMs) encompass a diverse group of diseases characterized by considerable variability in clinical manifestations, antibody profiles, and responsiveness to immunosuppressive therapies. This study aimed to investigate the association between organ involvement and distinct myositis autoantibodies in individuals with IIM in a single-center cohort.
Patients with ICD diagnoses M33.1, M33.2, M33.9, or M609 who (1) had been tested with Euroline blot assay for myositis autoantibodies and (2) met the classification criteria of definite/probable polymyositis (PM) or dermatomyositis (DM), anti-synthetase syndrome (ASS), or inclusion body myositis (IBM) were included. Medical journals were retrospectively examined with respect to clinical disease features.
Seventy patients (median age 58 years; 66% females) were included and represented the following diagnosis: PM ( = 23), DM ( = 21), ASS ( = 23), and IBM ( = 3). Most of the patients (87%) presented a muscle biopsy indicative of myositis. The presence of autoantibodies was as follows: myositis-specific antibodies, MSA ( = 53), myositis-associated antibodies, MAA ( = 33), both MSA + MAA ( = 24), MSA only ( = 29), MAA only ( = 9), no MSA, or MAA ( = 8). Anti-Jo-1 was the most common MSA (19%), whereas the most common MAA was anti-Ro/SSA52 (31%). We observed a significant association between antibody patterns and lung disease. In our cohort, 47% of the patients in the whole study group, 86% of patients with anti-SSA52, and 100% with anti-Jo-1 had pulmonary involvement. Patients with both MSA and MAA had a higher incidence of lung disease and decreased CO-diffusion capacity. This was especially prominent in anti-Ro/SSA52-positive patients. Interestingly, none of the patients suffered from lung disease if only antibodies against Mi-2α, Mi-2β, NXP2, HMGCR, and TIF1γ were present or no MSA/MAA were detected.
The simultaneous presence of both MAA and MSA indicates an increased risk of lung involvement in patients with inflammatory myopathies. The presence of any MAA, and especially anti-Ro/SSA52, is associated with more severe pulmonary disease. Our data suggest that MAA antibodies might be relevant markers for early detection and treatment of lung involvement in IIM.
特发性炎性肌病(IIMs)是一组多样的疾病,其临床表现、抗体谱以及对免疫抑制治疗的反应存在很大差异。本研究旨在调查单中心队列中IIM患者器官受累情况与不同肌炎自身抗体之间的关联。
纳入国际疾病分类(ICD)诊断为M33.1、M33.2、M33.9或M609的患者,这些患者需满足以下条件:(1)已通过Euroline印迹法检测肌炎自身抗体;(2)符合确诊/可能的多发性肌炎(PM)、皮肌炎(DM)、抗合成酶综合征(ASS)或包涵体肌炎(IBM)的分类标准。回顾性查阅医学期刊以获取临床疾病特征。
共纳入70例患者(中位年龄58岁;66%为女性),诊断如下:PM(n = 23)、DM(n = 21)、ASS(n = 23)和IBM(n = 3)。大多数患者(87%)的肌肉活检显示为肌炎。自身抗体的存在情况如下:肌炎特异性抗体(MSA,n = 53)、肌炎相关抗体(MAA,n = 33)、MSA + MAA两者皆有(n = 24)、仅MSA(n = 29)、仅MAA(n = 9)、无MSA或MAA(n = 8)。抗Jo - 1是最常见的MSA(19%),而最常见的MAA是抗Ro/SSA52(31%)。我们观察到抗体模式与肺部疾病之间存在显著关联。在我们的队列中,整个研究组47%的患者、抗SSA52患者中的86%以及抗Jo - 1患者中的100%有肺部受累。同时有MSA和MAA的患者肺部疾病发生率更高且一氧化碳弥散能力降低。这在抗Ro/SSA52阳性患者中尤为突出。有趣的是,如果仅存在针对Mi - 2α、Mi - 2β、NXP2、HMGCR和TIF1γ的抗体或未检测到MSA/MAA,则没有患者患有肺部疾病。
MAA和MSA同时存在表明炎性肌病患者肺部受累风险增加。任何MAA的存在,尤其是抗Ro/SSA52,与更严重的肺部疾病相关。我们的数据表明,MAA抗体可能是IIM患者肺部受累早期检测和治疗的相关标志物。
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