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The interleukin 17 system in cortical lesions in focal cortical dysplasias

机译:白细胞介素17系统在局灶性皮质发育不良的皮质病变中的作用

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Focal cortical dysplasias (FCDs) are increasingly recognized as important causes of medically intractable epilepsy. To understand the potential role of the interleukin 17 (IL-17) system in the epileptogenesis of FCDs, we studied the expression patterns of the IL-17 system in 15 FCD type Ia (FCDIa), 12 FCD type IIa (FCDIIa), and 12 FCD type IIb (FCDIIb) cortical lesions and compared the results with those in cerebral cortex from 10 control patients. Protein levels of IL-17, IL-17 receptor (IL-17R), and downstream factors of the IL-17 pathway (nuclear factor-??B activator 1 [NF??B; ACT1] and NF??B-p65) were markedly elevated in FCDIa, FCDIIa, and FCDIIb. Moreover, protein levels of IL-17 and IL-17R positively correlated with the frequency of seizures in FCD patients. Immunostaining indicated that IL-17 and IL-17R are highly expressed in neuronal microcolumns, dysmorphic neurons, balloon cells, astrocytes, and vascular endothelial cells. Nuclear factor-??B activator 1 and NF??B-p65 were diffusely expressed in FCDs. In addition, we detected a few IL-17-positive, CD4-positive T lymphocytes in FCDIIa and FCDIIb but not in FCDIa. Taken together, these findings suggest that the overexpression of the IL-17 system and the activation of the IL-17 signal transduction pathway may be involved in the epileptogenicity ofcortical lesions in FCDs, thus representing a novel potential target for antiepileptic therapy. ? 2013 by the American Association of Neuropathologists, Inc.
机译:局灶性皮质发育异常(FCD)日益被认为是医学上难治的癫痫的重要原因。为了解白介素17(IL-17)系统在FCD癫痫发生中的潜在作用,我们研究了IL-17系统在15种FCD Ia(FCDIa),12种FCD IIa(FCDIIa)中的表达模式。将12个FCD IIb型(FCDIIb)皮质病变与10例对照患者的大脑皮层结果进行比较。 IL-17,IL-17受体(IL-17R)和IL-17途径的下游因子(核因子-ΔβB激活剂1 [NFΔβ; ACT1]和NFΔβ-p65)的蛋白水平)在FCDIa,FCDIIa和FCDIIb中明显升高。此外,IL-17和IL-17R的蛋白质水平与FCD患者的癫痫发作频率呈正相关。免疫染色表明,IL-17和IL-17R在神经元微柱,畸形神经元,球囊细胞,星形胶质细胞和血管内皮细胞中高表达。核因子-βB激活剂1和NFβB-p65在FCD中分散表达。此外,我们在FCDIIa和FCDIIb中检测到一些IL-17阳性,CD4阳性T淋巴细胞,但在FCDIa中未检测到。综上所述,这些发现表明IL-17系统的过表达和IL-17信号转导途径的激活可能与FCDs皮质损伤的致癫痫性有关,因此代表了抗癫痫治疗的新的潜在靶标。 ?美国神经病理学家协会,2013年。

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