Prevalence and Clinical Implications of Autoantibodies in Juvenile Dermatomyositis: A Single-Center Experience From India.

IF 2.4 4区医学 Q2 RHEUMATOLOGY

JCR: Journal of Clinical Rheumatology Pub Date : 2024-10-01 Epub Date: 2024-08-22 DOI:10.1097/RHU.0000000000002127

Alen Joe Joseph, Baehat Dhakal, Sathvik Reddy Erla, Yogendra Singh, Lata Singh, Ashish D Upadhyay, Narendra Kumar Bagri, Rakesh Lodha, S K Kabra

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引用次数: 0

Abstract

Objective: This study aimed to characterize the profile of myositis-specific and myositis-associated autoantibodies (MSAs/MAAs) in an Indian cohort of juvenile dermatomyositis (JDM) patients and correlate them with clinical features and outcomes.

Methods: Forty-three children diagnosed with JDM were enrolled for this observational study. Clinical details (presentation, course, and outcome) were noted in a predesigned proforma. Serum samples were tested for 16 MSAs/MAAs by line immunoassay. MSAs/MAAs were correlated with clinical features and outcome (defined as a complete clinical response [≥6 months' disease inactivity on medication] or complete remission [≥6 months' inactivity off all drugs]).

Results: Thirty-five subjects (81.4%) had at least 1 MSA/MAA detected. The most common antibodies were anti-NXP2 (n = 13, 30.2%), anti-TIF1γ (n = 10, 23.2%), and anti-MDA-5 (n = 8, 18.6%). No patient had anti-Ku, anti-Pm Scl-100, anti-PL-12, anti-EJ, anti-OJ, or anti-Ro52. Thirty-two patients (74.4%) attained a complete clinical response over a median follow-up duration of 14 months, among which 6 (13.9%) achieved complete remission over a median follow-up duration of 30 months. Anti-TIF1γ was associated with younger age at onset (≤3 years) (odds ratio [OR], 6.25; 95% confidence interval [CI], 1.15-34.12; p = 0.034) and disease flares after attaining complete response (OR, 10.18; 95% CI, 1.64-70.93; p = 0.013). Patients with anti-NXP2 had higher odds of severe muscular weakness (OR, 3.73; 95% CI, 0.95-14.59; p = 0.058) and truncal weakness (OR, 3.89; 95% CI, 0.97-15.64; p = 0.056). One child with anti-MDA-5 positivity had interstitial lung disease. We found no association between the MSA/MAA profile and the achievement of complete clinical response or remission.

Conclusions: MSAs/MAAs were identified in 81% of children with JDM in our study, which is higher than most other studies. The most frequently observed antibodies displayed a pattern consistent with other studies. Anti-TIF1γ was associated with a younger age at onset and disease flares even after attaining a complete clinical response. Anti-NXP2 had higher odds of severe muscular weakness. These observations suggest consistency in certain phenotypic associations observed across geographic boundaries.

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自身抗体在幼年皮肌炎中的流行情况和临床意义：印度单中心经验

研究目的本研究旨在描述印度幼年皮肌炎（JDM）患者中肌炎特异性和肌炎相关自身抗体（MSA/MAAs）的特征，并将其与临床特征和预后相关联：这项观察性研究招募了43名确诊为幼年皮肌炎的儿童。在预先设计的表格中记录了临床细节（表现、病程和结果）。血清样本通过线性免疫测定法检测了16种MSA/MAAs。MSA/MAAs与临床特征和结果（定义为完全临床反应[服药≥6个月无症状]或完全缓解[停药≥6个月无症状]）相关：35名受试者（81.4%）至少检测到一种MSA/MAA。最常见的抗体是抗 NXP2（13 例，30.2%）、抗 TIF1γ （10 例，23.2%）和抗 MDA-5 （8 例，18.6%）。没有患者出现抗Ku、抗Pm Scl-100、抗PL-12、抗EJ、抗OJ或抗Ro52。32名患者（74.4%）在14个月的中位随访期间获得了完全临床应答，其中6名患者（13.9%）在30个月的中位随访期间获得了完全缓解。抗TIF1γ与发病年龄较小（≤3岁）（几率比[OR]，6.25；95% 置信区间[CI]，1.15-34.12；P = 0.034）和获得完全应答后疾病复发（OR，10.18；95% CI，1.64-70.93；P = 0.013）有关。抗NXP2患者出现重症肌无力（OR，3.73；95% CI，0.95-14.59；p = 0.058）和肢体无力（OR，3.89；95% CI，0.97-15.64；p = 0.056）的几率更高。一名抗MDA-5阳性患儿患有间质性肺病。我们发现，MSA/MAA特征与完全临床反应或缓解之间没有关联：在我们的研究中，81%的JDM患儿体内发现了MSA/MAA，高于其他大多数研究。最常观察到的抗体显示出与其他研究一致的模式。抗TIF1γ与较小的发病年龄和疾病复发有关，即使在获得完全临床应答后也是如此。抗 NXP2 导致重症肌无力的几率更高。这些观察结果表明，跨地域观察到的某些表型关联具有一致性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

JCR: Journal of Clinical Rheumatology 医学-风湿病学

CiteScore

3.50

自引率

2.90%

发文量

228

审稿时长

4-8 weeks

期刊介绍： JCR: Journal of Clinical Rheumatology the peer-reviewed, bimonthly journal that rheumatologists asked for. Each issue contains practical information on patient care in a clinically oriented, easy-to-read format. Our commitment is to timely, relevant coverage of the topics and issues shaping current practice. We pack each issue with original articles, case reports, reviews, brief reports, expert commentary, letters to the editor, and more. This is where you''ll find the answers to tough patient management issues as well as the latest information about technological advances affecting your practice.