新生雌二醇刺激可预防 X 连锁婴儿痉挛综合征 Arx 模型中的癫痫。
Neonatal estradiol stimulation prevents epilepsy in Arx model of X-linked infantile spasms syndrome.
机构信息
Blue Bird Circle Developmental Neurogenetics Laboratory, Department of Neurology, Baylor College of Medicine, Houston, TX 77030, USA.
出版信息
Sci Transl Med. 2014 Jan 22;6(220):220ra12. doi: 10.1126/scitranslmed.3007231.
Abstract
Infantile spasms are a catastrophic form of pediatric epilepsy with inadequate treatment. In patients, mutation of ARX, a transcription factor selectively expressed in neuronal precursors and adult inhibitory interneurons, impairs cell migration and causes a major inherited subtype of the disease X-linked infantile spasms syndrome. Using an animal model, the Arx((GCG)10+7) mouse, we determined that brief estradiol (E2) administration during early postnatal development prevented spasms in infancy and seizures in adult mutants. E2 was ineffective when delivered after puberty or 30 days after birth. Early E2 treatment altered mRNA levels of three downstream targets of Arx (Shox2, Ebf3, and Lgi1) and restored depleted interneuron populations without increasing GABAergic synaptic density. Postnatal E2 treatment may induce lasting transcriptional changes that lead to enduring disease modification and could potentially serve as a therapy for inherited interneuronopathies.
摘要
婴儿痉挛症是一种治疗效果不佳的儿童癫痫灾难性形式。在患者中,选择性表达于神经元前体细胞和成年抑制性中间神经元的转录因子 ARX 的突变会损害细胞迁移,并导致疾病的一个主要遗传性亚型 X 连锁婴儿痉挛综合征。我们使用一种动物模型 Arx((GCG)10+7 小鼠,确定了在早期新生后发育期间给予短暂的雌二醇 (E2) 治疗可预防婴儿痉挛和成年突变体的癫痫发作。在青春期后或出生后 30 天给予 E2 则无效。早期 E2 治疗改变了 ARX 的三个下游靶标(Shox2、Ebf3 和 Lgi1)的 mRNA 水平,并恢复了耗竭的中间神经元群体,而没有增加 GABA 能突触密度。出生后 E2 治疗可能会诱导持久的转录变化,从而导致持久的疾病修饰,并可能成为遗传性中间神经元病的一种治疗方法。
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