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首页> 外文期刊>Brain & Development >Expression of TRPV1 in cortical lesions from patients with tuberous sclerosis complex and focal cortical dysplasia type IIb
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Expression of TRPV1 in cortical lesions from patients with tuberous sclerosis complex and focal cortical dysplasia type IIb

机译:TRPV1在结节性硬化症合并IIb型局灶性皮质发育异常患者皮质病变中的表达

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Tuberous sclerosis complex (TSC) and focal cortical dysplasia type IIb (FCDIIb) are recognized as causes of intractable epilepsy. Transient receptor potential vanilloid receptor 1 (TRPV1), a member of the transient receptor potential family, is the capsaicin receptor and is known to be involved in peripheral nociception. Recent evidence suggested that TRPV1 may be a contributing factor in epileptogenicity. Here, we evaluated the expression of TRPV1 in the cortical lesions of TSC and FCDIIb relative to normal control cortex. TRPV1 was studied in epilepsy surgery cases with TSC (cortical tubers; n= 12) and FCDIIb (n= 12) using immunocytochemistry, confocal analysis, and Western blotting (WB). Immunohistochemical location of the TRPV1 was predominately detected in the abnormal cell types, such as dysmorphic neurons, balloon cells (BCs) and giant cells. Co-localization assays further revealed that cells expressing TRPV1 mainly had a neuronal lineage, apart from some BCs in FCDIIb, which obviously were of astrocytic lineage. The increased TRPV1 expression within the dysplastic cortex of TSC and FCDIIb was confirmed by WB. Interestingly, both immunohistochemical and WB data indicated that TRPV1 might have both cytoplasm and nuclear distribution, suggesting a potential nuclear role of TRPV1. The over-expression of TRPV1 in cortical lesions of TSC and FCDIIb suggested the possible involvement of TRPV1 in the intrinsic and increased epileptogenicity of malformations of cortical development associated epilepsy diseases and may represent a potential antiepileptogenic target. However, the current data are merely descriptive, and further electrophysiological investigation is needed in the future.
机译:结节性硬化复合物(TSC)和局灶性皮质发育异常IIb型(FCDIIb)被认为是顽固性癫痫的原因。瞬时受体电位类香草酸受体1(TRPV1)是瞬时受体电位家族的成员,是辣椒素受体,已知与周围伤害感受有关。最近的证据表明TRPV1可能是致痫性的一个因素。在这里,我们评估了相对于正常对照皮质,TSC和FCDIIb皮质病变中TRPV1的表达。使用免疫细胞化学,共聚焦分析和蛋白质印迹(WB)在TSC(皮质块茎; n = 12)和FCDIIb(n = 12)的癫痫手术病例中研究了TRPV1。在异常细胞类型中,主要检测到TRPV1的免疫组织化学位置,例如畸形神经元,球囊细胞(BCs)和巨细胞。共定位分析进一步揭示了表达TRPV1的细胞主要具有神经元谱系,除了FCDIIb中的某些BC明显属于星形细胞谱系。 WB证实了TSC和FCDIIb的发育异常皮质内TRPV1表达的增加。有趣的是,免疫组化和WB数据均表明TRPV1可能同时具有细胞质和核分布,提示TRPV1具有潜在的核作用。 TPV和FCDIIb皮质病变中TRPV1的过度表达提示TRPV1可能参与了与皮质发育相关的癫痫病畸形的内在和增加的致癫痫性,并且可能代表了潜在的抗癫痫目标。但是,当前数据仅是描述性的,将来需要进一步的电生理研究。

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