临床疑似血清阴性自身免疫相关性癫痫患者的细胞因子谱改变

Katherine Motovilov, Cole Maguire, Deborah Briggs, Esther Melamed
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摘要

背景和目的自身免疫相关性癫痫(AAE)是一种对免疫疗法反应良好但对传统抗癫痫干预措施反应不佳的疾病,它正在成为耐药性癫痫病例的重要诱因。目前的 AAE 诊断标准依赖于筛查患者血清或脑脊液中已知的神经元自身抗体。然而,这种诊断方法无法捕捉到对免疫疗法有反应但已知自身抗体血清阴性(snAAE)的疑似 AAE 耐药癫痫患者。方法为了确定snAAE的潜在生物标志物,我们评估了迄今为止最全面的细胞因子和自身抗体检测组合,比较了snAAE患者、抗癫痫药物(ASM)反应性癫痫患者和其他神经炎症性疾病患者。结果我们发现,snAAE 患者体内有 14 种细胞因子明显升高的独特特征,包括GM-CSF、MCP-2/CCL8、MIP-1a/CCL3、IL-1RA、IL-6、IL-8、IL-9、IL-10、IL-15、IL-20、VEGF-A、TNF-b、LIF 和 TSLP。根据先前的文献,我们强调 IL-6、IL-8、IL-10、IL-13、VEGF-A 和 TNF-b 是 snAAE 潜在的可操作细胞因子生物标记物,它们在 snAAE 患者的临床评估中可能具有诊断作用。自身抗体组筛选未能在snAAE患者中发现针对神经元通道蛋白的自身抗体。有趣的是,ASM反应性癫痫患者中针对脑浆膜蛋白的自身抗体比例升高,这可能表明尽管癫痫发作活动控制良好,但患者仍存在免疫亢进/功能障碍,并提示ASM反应性患者可能经历独立于癫痫发作活动的疾病进展(PISA)。讨论总之,我们的研究结果表明,仅仅扩大现有的自身抗体筛查范围可能不足以提高snAAE的诊断能力。相反,我们建议细胞因子分析可作为一种有前途的诊断途径,用于识别 AAE 患者的免疫失调,并为免疫疗法试验提供机会。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Altered Cytokine Profile in Clinically Suspected Seronegative Autoimmune Associated Epilepsy
Background and Objectives Autoimmune-associated epilepsy (AAE), a condition which responds favorably to immune therapies but not traditional anti-seizure interventions, is emerging as a significant contributor to cases of drug-resistant epilepsy. Current standards for the diagnosis of AAE rely on screening for known neuronal autoantibodies in patient serum or cerebrospinal fluid. However, this diagnostic method fails to capture a subset of drug-resistant epilepsy patients with suspected AAE who respond to immunotherapy yet remain seronegative (snAAE) for known autoantibodies. Methods To identify potential biomarkers for snAAE, we evaluated the most comprehensive panel of assayed cytokines and autoantibodies to date, comparing patients with snAAE, anti-seizure medication (ASM) responsive epilepsy, and patients with other neuroinflammatory diseases. Results We found a unique signature of 14 cytokines significantly elevated in snAAE patients including: GM-CSF, MCP-2/CCL8, MIP-1a/CCL3, IL-1RA, IL-6, IL-8, IL-9, IL-10, IL-15, IL-20, VEGF-A, TNF-b, LIF, and TSLP. Based on prior literature, we highlight IL-6, IL-8, IL-10, IL-13, VEGF-A, and TNF-b as potentially actionable cytokine biomarkers for snAAE, which could be of diagnostic utility in clinical evaluations of snAAE patients. Autoantibody-ome screening failed to identify autoantibodies targeting neuronal channel proteins in snAAE patients. Interestingly, ASM-responsive epilepsy patients displayed elevations in the proportion of autoantibodies targeting brain plasma membrane proteins, possibly pointing to the presence of immune hyperactivity/dysfunction despite well-controlled seizure activity and suggesting ASM-responsive patients may experience disease progression independent of seizure activity (PISA). Discussion Overall, our findings suggest that simply expanding existing autoantibody screens may not sufficiently enhance diagnostic power for snAAE. Instead, we propose that cytokine analysis may serve as a promising diagnostic avenue for identifying immune dysregulation in AAE patients and enabling opportunities for trials of immunotherapies.
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