Department of Neurology, Medical Faculty and University Hospital Düsseldorf, Heinrich Heine University, Moorenstr. 5, 40225, Düsseldorf, Germany.
Department of Neurology, Charité - Universitätsmedizin Berlin, 10117, Berlin, Germany.
Acta Neuropathol. 2024 Jun 18;147(1):102. doi: 10.1007/s00401-024-02754-6.
Myasthenia gravis is a chronic antibody-mediated autoimmune disease disrupting neuromuscular synaptic transmission. Informative biomarkers remain an unmet need to stratify patients with active disease requiring intensified monitoring and therapy; their identification is the primary objective of this study. We applied mass spectrometry-based proteomic serum profiling for biomarker discovery. We studied an exploration and a prospective validation cohort consisting of 114 and 140 anti-acetylcholine receptor antibody (AChR-Ab)-positive myasthenia gravis patients, respectively. For downstream analysis, we applied a machine learning approach. Protein expression levels were confirmed by ELISA and compared to other myasthenic cohorts, in addition to myositis and neuropathy patients. Anti-AChR-Ab levels were determined by a radio receptor assay. Immunohistochemistry and immunofluorescence of intercostal muscle biopsies were employed for validation in addition to interactome studies of inter-alpha-trypsin inhibitor heavy chain H3 (ITIH3). Machine learning identified ITIH3 as potential serum biomarker reflective of disease activity. Serum levels correlated with disease activity scores in the exploration and validation cohort and were confirmed by ELISA. Lack of correlation between anti-AChR-Ab levels and clinical scores underlined the need for biomarkers. In a subgroup analysis, ITIH3 was indicative of treatment responses. Immunostaining of muscle specimens from these patients demonstrated ITIH3 localization at the neuromuscular endplates in myasthenia gravis but not in controls, thus providing a structural equivalent for our serological findings. Immunoprecipitation of ITIH3 and subsequent proteomics lead to identification of its interaction partners playing crucial roles in neuromuscular transmission. This study provides data on ITIH3 as a potential pathophysiological-relevant biomarker of disease activity in myasthenia gravis. Future studies are required to facilitate translation into clinical practice.
重症肌无力是一种慢性抗体介导的自身免疫性疾病,破坏神经肌肉突触传递。有意义的生物标志物仍然是未满足的需求,以分层需要强化监测和治疗的活动性疾病患者;它们的鉴定是这项研究的主要目标。我们应用基于质谱的蛋白质组血清分析进行生物标志物发现。我们研究了一个探索性和一个前瞻性验证队列,分别由 114 名和 140 名抗乙酰胆碱受体抗体(AChR-Ab)阳性重症肌无力患者组成。对于下游分析,我们应用了机器学习方法。通过 ELISA 确认蛋白质表达水平,并与其他肌无力队列以及肌炎和神经病患者进行比较。抗 AChR-Ab 水平通过放射性受体测定法确定。免疫组化和免疫荧光染色用于肋间肌活检的验证,此外还进行了抗胰蛋白酶抑制剂重链 H3(ITIH3)的互作组研究。机器学习确定 ITIH3 为潜在的反映疾病活动的血清生物标志物。在探索性和验证队列中,血清水平与疾病活动评分相关,并通过 ELISA 得到证实。抗 AChR-Ab 水平与临床评分之间缺乏相关性,强调了对生物标志物的需求。在亚组分析中,ITIH3 提示治疗反应。来自这些患者的肌肉标本的免疫染色显示 ITIH3 在重症肌无力中的神经肌肉终板处定位,但在对照组中没有,从而为我们的血清学发现提供了结构等价物。ITIH3 的免疫沉淀和随后的蛋白质组学导致鉴定出其在神经肌肉传递中发挥关键作用的相互作用伙伴。这项研究提供了 ITIH3 作为重症肌无力疾病活动潜在病理生理相关生物标志物的相关数据。需要进一步的研究将其转化为临床实践。
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