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首页> 外文期刊>Human Molecular Genetics >Neurodevelopmental defects resulting from ATRX overexpression in transgenic mice.
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Neurodevelopmental defects resulting from ATRX overexpression in transgenic mice.

机译:由ATRX在转基因小鼠中过度表达导致的神经发育缺陷。

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Several X-linked mental retardation syndromes are caused by mutations in the ATRX gene. Common clinical features associated with ATRX mutations include severe mental retardation, characteristic facial anomalies and variable degrees of urogenital defects and alpha-thalassemia. Although the ATRX protein is a member of the SWI/SNF family of chromatin remodeling proteins, little is known about the biochemical activity of the ATRX protein or its in vivo function during development. Here we demonstrate that ATRX is part of a large multiprotein complex similar in size to the SWI/SNF complex. Furthermore, we have generated transgenic mice that overexpress ATRX as an initial model for studying the function of this protein during development. Misexpression of ATRX was associated with growth retardation, neural tube defects and a high incidence of embryonic death. Moreover, brains from E10.5 transgenic embryos displayed abnormal growth and organization of the ventricular zone that was highly convoluted in the most severely affected embryos. Transgenic mice that survived to birth exhibited a high incidence of perinatal death, as well as seizures, mild craniofacial anomalies and abnormal behavior. Our findings indicate that ATRX dosage is crucial for normal development and organization of the cortex, and emphasize the relevance of our model for the study of ATRX function and disease pathogenesis.
机译:一些X连锁的智力低下综合征是由ATRX基因的突变引起的。与ATRX突变相关的常见临床特征包括严重的智力低下,特征性的面部异常以及可变程度的泌尿生殖系统缺陷和α地中海贫血。尽管ATRX蛋白是染色质重塑蛋白的SWI / SNF家族的成员,但对于ATRX蛋白的生化活性或其在发育过程中的体内功能了解甚少。在这里,我们证明ATRX是大型多蛋白复合物的一部分,其大小与SWI / SNF复合物相似。此外,我们已经产生了过表达ATRX的转基因小鼠,作为研究该蛋白在发育过程中功能的初始模型。 ATRX的错误表达与生长迟缓,神经管缺陷和胚胎死亡的高发有关。此外,来自E10.5转基因胚胎的大脑显示出异常的生长和心室区的组织,在受影响最严重的胚胎中该区高度回旋。存活到出生的转基因小鼠表现出高的围产期死亡,癫痫发作,轻度颅面畸形和异常行为。我们的发现表明,ATRX剂量对于皮质的正常发育和组织至关重要,并强调了我们的模型与ATRX功能和疾病发病机制研究的相关性。

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