在局灶性皮质发育不良 IIb 型和结节性硬化症患者的致痫灶中,甲酰肽受体 2 的表达下调。
Downregulated formyl peptide receptor 2 expression in the epileptogenic foci of patients with focal cortical dysplasia type IIb and tuberous sclerosis complex.
机构信息
Department of Neurosurgery, Epilepsy Research Center of PLA, Xinqiao Hospital, Army Medical University (Third Military Medical University), Chongqing, China.
Department of Neurosurgery, Armed Police Hospital of Chongqing, Chongqing, China.
出版信息
Immun Inflamm Dis. 2022 Nov;10(11):e706. doi: 10.1002/iid3.706.
BACKGROUND
Focal cortical dysplasia type IIb (FCDIIb) and tuberous sclerosis complex (TSC) show persistent neuroinflammation, which promotes epileptogenesis and epilepsy progression, suggesting that endogenous resolution of inflammation is inadequate to relieve neuronal network hyperexcitability. To explore the potential roles of formyl peptide receptor 2 (FPR2), which is a key regulator of inflammation resolution, in epilepsy caused by FCDIIb and TSC, we examined the expression and cellular distribution of FPR2.
METHOD
The expression of FPR2 and nuclear factor-κB (NF-κB) signaling pathway was examined by real-time PCR, western blots, and analyzed via one-way analysis of variance. The distribution of FPR2 was detected using immunostaining. The expression of resolvin D1 (RvD1, the endogenous ligand of FPR2) was observed via enzyme-linked immunosorbent assay. Pearson's correlation test was used to evaluate the correlation between the expression levels of FPR2 and RvD1 and the clinical variants.
RESULTS
The expression of FPR2 was significantly lower in FCDIIb (p = .0146) and TSC (p = .0006) cortical lesions than in controls, as was the expression of RvD1 (FCDIIb: p = .00431; TSC: p = .0439). Weak FPR2 immunoreactivity was observed in dysmorphic neurons (DNs), balloon cells (BCs), and giant cells (GCs) in FCDIIb and TSC tissues. Moreover, FPR2 was mainly distributed in dysplastic neurons; it was sparse in microglia and nearly absent in astrocytes. The NF-κB pathway was significantly activated in patients with FCDIIb and TSC, and the protein level of NF-κB was negatively correlated with the protein level of FPR2 (FCDIIb: p = .00395; TSC: p = .0399). In addition, the protein level of FPR2 was negatively correlated with seizure frequency in FCDIIb (p = .0434) and TSC (p = .0351) patients.
CONCLUSION
In summary, these results showed that the expression and specific distribution of FPR2 may be involved in epilepsy caused by FCDIIb and TSC, indicating that downregulation of FPR2 mediated the dysfunction of neuroinflammation resolution in FCDIIb and TSC.
背景
局灶性皮质发育不良 IIb 型(FCDIIb)和结节性硬化症(TSC)表现出持续的神经炎症,这促进了癫痫的发生和进展,表明内源性炎症消退不足以缓解神经元网络的过度兴奋。为了探讨作为炎症消退关键调节剂的甲酰肽受体 2(FPR2)在 FCDIIb 和 TSC 引起的癫痫中的潜在作用,我们检查了 FPR2 的表达和细胞分布。
方法
通过实时 PCR、Western blot 检测 FPR2 和核因子-κB(NF-κB)信号通路的表达,并进行单因素方差分析。通过免疫染色检测 FPR2 的分布。通过酶联免疫吸附试验观察内源性配体 RvD1(FPR2 的内源性配体)的表达。采用皮尔逊相关检验评估 FPR2 和 RvD1 的表达水平与临床变异的相关性。
结果
FCDIIb(p=0.0146)和 TSC(p=0.0006)皮质病变中 FPR2 的表达明显低于对照组,RvD1 的表达也明显低于对照组(FCDIIb:p=0.00431;TSC:p=0.0439)。FCDIIb 和 TSC 组织中的畸形神经元(DNs)、气球细胞(BCs)和巨细胞(GCs)中观察到微弱的 FPR2 免疫反应性。此外,FPR2 主要分布在发育不良的神经元中;在小胶质细胞中稀疏,在星形胶质细胞中几乎不存在。FCDIIb 和 TSC 患者的 NF-κB 通路明显激活,NF-κB 蛋白水平与 FPR2 蛋白水平呈负相关(FCDIIb:p=0.00395;TSC:p=0.0399)。此外,FPR2 蛋白水平与 FCDIIb 患者的癫痫发作频率呈负相关(p=0.0434)和 TSC 患者的癫痫发作频率呈负相关(p=0.0351)。
结论
总之,这些结果表明,FPR2 的表达和特定分布可能参与了 FCDIIb 和 TSC 引起的癫痫,表明 FCDIIb 和 TSC 中 FPR2 下调介导了神经炎症消退功能障碍。
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