活动性重症神经精神性系统性红斑狼疮中神经元和神经胶质损伤的血液生物标志物
Blood-based biomarkers of neuronal and glial injury in active major neuropsychiatric systemic lupus erythematosus.
作者信息
Kammeyer Ryan, Chapman Kimberly, Furniss Anna, Hsieh Elena, Fuhlbrigge Robert, Ogbu Ekemini A, Boackle Susan, Zell JoAnn, Nair Kavita V, Borko Tyler L, Cooper Jennifer C, Bennett Jeffrey L, Piquet Amanda L
机构信息
Departments of Pediatrics and Neurology, University of Colorado School of Medicine, Aurora, CO, USA.
Department of Neurology, University of Colorado School of Medicine, Aurora, CO, USA.
出版信息
Lupus. 2024 Sep;33(10):1116-1129. doi: 10.1177/09612033241272961. Epub 2024 Aug 16.
BACKGROUND
Neuropsychiatric systemic lupus erythematosus (NPSLE) is a poorly understood and heterogeneous manifestation of SLE. Common major NPSLE syndromes include strokes, seizures, myelitis, and aseptic meningitis. Easily obtainable biomarkers are needed to assist in early diagnosis and improve outcomes for NPSLE. A frequent end-result of major syndromes is neuronal or glial injury. Blood-based neurofilament light (NfL) and glial fibrillary acidic protein (GFAP) have been utilized as markers for monitoring disease activity and/or severity in other neurodegenerative and neuroinflammatory diseases; however, they have not been evaluated in active major NPSLE.
METHODS
This was a case-control study. We enrolled patients aged 12-60 years with active major NPSLE, SLE without active major NPSLE, and healthy controls. Active NPSLE was defined as being <6 months from last new or worsening neuropsychiatric symptom. Demographics, clinical data, and serum or plasma biosamples were collected.
RESULTS
Thirteen patients with active major NPSLE, 13 age/sex/kidney function matched SLE controls without active major NPSLE, and 13 age/sex matched healthy controls (mean ages 26.8, 27.3, 26.6 years) were included. 92% of each group were female. Major syndromes included stroke (5), autonomic disorder (3), demyelinating disease (2), aseptic meningitis (2), sensorimotor polyneuropathy (2), cranial neuropathy (1), seizures (1), and myelopathy (2). Mean (standard deviation) blood NfL and GFAP were 3.6 pg/ml (2.0) and 50.4 pg/ml (15.0), respectively, for the healthy controls. Compared to healthy controls, SLE without active major NPSLE had mean blood NfL and GFAP levels 1.3 pg/ml ( = .42) and 1.2 pg/ml higher ( = .53), respectively. Blood NfL was on average 17.9 pg/ml higher (95% CI: 9.2, 34.5; < .001) and blood GFAP was on average 3.2 pg/ml higher (95% CI: 1.9, 5.5; < .001) for cases of active major NPSLE compared to SLE without active major NPSLE. In a subset of 6 patients sampled at multiple time points, blood NfL and GFAP decreased after immunotherapy.
CONCLUSIONS
Blood NfL and GFAP levels are elevated in persons with SLE with active major NPSLE compared to disease matched controls and may lower after immunotherapy initiation. Larger and longitudinal studies are needed to ascertain their utility in a clinical setting.
背景
神经精神性系统性红斑狼疮(NPSLE)是系统性红斑狼疮(SLE)一种了解较少且异质性的表现形式。常见的主要NPSLE综合征包括中风、癫痫发作、脊髓炎和无菌性脑膜炎。需要易于获取的生物标志物来辅助NPSLE的早期诊断并改善其预后。主要综合征的一个常见最终结果是神经元或神经胶质损伤。基于血液的神经丝轻链(NfL)和胶质纤维酸性蛋白(GFAP)已被用作监测其他神经退行性和神经炎性疾病的疾病活动和/或严重程度的标志物;然而,它们尚未在活动性主要NPSLE中进行评估。
方法
这是一项病例对照研究。我们纳入了年龄在12 - 60岁之间的活动性主要NPSLE患者、无活动性主要NPSLE的SLE患者以及健康对照。活动性NPSLE被定义为距离上次出现新的或恶化的神经精神症状小于6个月。收集了人口统计学、临床数据以及血清或血浆生物样本。
结果
纳入了13例活动性主要NPSLE患者、13例年龄/性别/肾功能匹配的无活动性主要NPSLE的SLE对照以及13例年龄/性别匹配的健康对照(平均年龄分别为26.8岁、27.3岁、26.6岁)。每组中92%为女性。主要综合征包括中风(5例)、自主神经功能障碍(3例)、脱髓鞘疾病(2例)、无菌性脑膜炎(2例)、感觉运动性多发性神经病(2例)、颅神经病变(1例)、癫痫发作(1例)和脊髓病(2例)。健康对照的血液NfL和GFAP平均(标准差)分别为3.6 pg/ml(2.0)和50.4 pg/ml(15.0)。与健康对照相比,无活动性主要NPSLE的SLE患者血液NfL和GFAP水平分别高1.3 pg/ml(P = 0.42)和1.2 pg/ml(P = 0.53)。与无活动性主要NPSLE的SLE患者相比,活动性主要NPSLE患者的血液NfL平均高17.9 pg/ml(95%可信区间:9.2,34.5;P < 0.001),血液GFAP平均高3.2 pg/ml(95%可信区间:1.9,5.5;P < 0.001)。在6例多个时间点采样的亚组患者中,免疫治疗后血液NfL和GFAP下降。
结论
与疾病匹配的对照相比,患有活动性主要NPSLE的SLE患者血液NfL和GFAP水平升高,且在开始免疫治疗后可能降低。需要进行更大规模的纵向研究以确定它们在临床环境中的效用。
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