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首页> 外文期刊>Scientific reports. >High-throughput screen detects calcium signaling dysfunction in typical sporadic autism spectrum disorder
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High-throughput screen detects calcium signaling dysfunction in typical sporadic autism spectrum disorder

机译:高通量屏幕检测典型的零星自闭症谱系疾病中的钙信号功能障碍

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Autism spectrum disorder (ASD) is a heterogeneous group of neurodevelopmental disorders without any defined uniting pathophysiology. Ca2+ signaling is emerging as a potential node in the genetic architecture of the disorder. We previously reported decreased inositol trisphosphate (IP3)-mediated Ca2+ release from the endoplasmic reticulum in several rare monogenic syndromes highly comorbid with autism – fragile X and tuberous sclerosis types 1 and 2 syndromes. We now extend those findings to a cohort of subjects with sporadic ASD without any known mutations. We developed and applied a high throughput Fluorometric Imaging Plate Reader (FLIPR) assay to monitor agonist-evoked Ca2+ signals in human primary skin fibroblasts. Our results indicate that IP3 -mediated Ca2+ release from the endoplasmic reticulum in response to activation of purinergic receptors is significantly depressed in subjects with sporadic as well as rare syndromic forms of ASD. We propose that deficits in IP3-mediated Ca2+ signaling represent a convergent hub function shared across the spectrum of autistic disorders – whether caused by rare highly penetrant mutations or sporadic forms – and holds promise as a biomarker for diagnosis and novel drug discovery.
机译:自闭症谱系障碍(ASD)是一种非均相神经发育疾病组,没有任何定义的致病病理学。 CA2 +信令作为疾病遗传架构中的潜在节点。我们之前报道的肌醇三种磷酸肌醇(IP3)介导的Ca2 +从内质子网中的几种罕见的单一综合征高度合并,具有自闭症 - 脆弱的X和肺结核硬化类型1和2综合征。我们现在将这些发现扩展到零星ASD的群体队列,而没有任何已知的突变。我们开发并应用了高吞吐量荧光成像板读取器(FLIPR)测定以监测人原发性皮肤成纤维细胞中的激动剂诱发的CA2 +信号。我们的结果表明,在散发性的受试者和罕见的综合征形式的ASD中,IP3介导的CA2 +从内质网的延伸的CA2 +释放。我们提出IP3介导的CA2 +信号传导中的缺陷代表了跨自闭症紊乱的频谱共享的会聚集线器函数 - 无论是由罕见的高度渗透突变或散发形式引起的 - 并持有诊断和新药发现的生物标志物。

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