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Exploratory Proteomic Analysis Implicates the Alternative Complement Cascade in Primary CNS Vasculitis

Neurology(2019)

Univ Calif San Francisco | Cleveland Clin | Boston Childrens Hosp | Connecticut Childrens Med Ctr | Univ Penn | Kaiser Permanente

Cited 14|Views66
Abstract
Objective To identify molecular correlates of primary angiitis of the CNS (PACNS) through proteomic analysis of CSF from a biopsy-proven patient cohort. Methods Using mass spectrometry, we quantitatively compared the CSF proteome of patients with biopsy-proven PACNS (n = 8) to CSF from individuals with noninflammatory conditions (n = 11). Significantly enriched molecular pathways were identified with a gene ontology workflow, and high confidence hits within enriched pathways (fold change >1.5 and concordant Benjamini-Hochberg-adjusted p < 0.05 on DeSeq and t test) were identified as differentially regulated proteins. Results Compared to noninflammatory controls, 283 proteins were differentially expressed in the CSF of patients with PACNS, with significant enrichment of the complement cascade pathway (C4-binding protein, CD55, CD59, properdin, complement C5, complement C8, and complement C9) and neural cell adhesion molecules. A subset of clinically relevant findings were validated by Western blot and commercial ELISA. Conclusions In this exploratory study, we found evidence of deregulation of the alternative complement cascade in CSF from biopsy-proven PACNS compared to noninflammatory controls. More specifically, several regulators of the C3 and C5 convertases and components of the terminal cascade were significantly altered. These preliminary findings shed light on a previously unappreciated similarity between PACNS and systemic vasculitides, especially anti-neutrophil cytoplasmic antibody-associated vasculitis. The therapeutic implications of this common biology and the diagnostic and therapeutic utility of individual proteomic findings warrant validation in larger cohorts.
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要点】:通过蛋白质组学分析,发现原发性中枢神经系统血管炎(PACNS)患者的脑脊液(CSF)中替代补体途径的异常激活。

方法】:使用质谱技术定量比较了经活检证实PACNS患者(n=8)的CSF蛋白质组与无炎症条件个体(n=11)的CSF蛋白质组。

实验】:实验中使用了质谱技术进行蛋白质定量分析,并在显著富集的分子通路中通过基因本体论工作流识别差异表达的蛋白质;通过Western blot和商业ELISA验证了部分临床相关发现。数据集为活检证实的PACNS患者和对照个体的CSF样本,发现283个蛋白质差异表达,其中补体途径显著富集,并在更大队列中验证了这些初步发现的治疗意义。