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首页> 外文期刊>The New England journal of medicine >A functional genetic link between distinct developmental language disorders.
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A functional genetic link between distinct developmental language disorders.

机译:不同发育语言障碍之间的功能遗传联系。

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摘要

BACKGROUND: Rare mutations affecting the FOXP2 transcription factor cause a monogenic speech and language disorder. We hypothesized that neural pathways downstream of FOXP2 influence more common phenotypes, such as specific language impairment. METHODS: We performed genomic screening for regions bound by FOXP2 using chromatin immunoprecipitation, which led us to focus on one particular gene that was a strong candidate for involvement in language impairments. We then tested for associations between single-nucleotide polymorphisms (SNPs) in this gene and language deficits in a well-characterized set of 184 families affected with specific language impairment. RESULTS: We found that FOXP2 binds to and dramatically down-regulates CNTNAP2, a gene that encodes a neurexin and is expressed in the developing human cortex. On analyzing CNTNAP2 polymorphisms in children with typical specific language impairment, we detected significant quantitative associations with nonsense-word repetition, a heritable behavioralmarker of this disorder (peak association, P=5.0x10(-5) at SNP rs17236239). Intriguingly, this region coincides with one associated with language delays in children with autism. CONCLUSIONS: The FOXP2-CNTNAP2 pathway provides a mechanistic link between clinically distinct syndromes involving disrupted language.
机译:背景:影响FOXP2转录因子的罕见突变会导致单基因语音和语言障碍。我们假设FOXP2下游的神经通路影响更常见的表型,例如特定的语言障碍。方法:我们使用染色质免疫沉淀对FOXP2结合的区域进行了基因组筛选,这使我们专注于一个特定的基因,该基因很可能参与语言障碍。然后,我们测试了该基因中的单核苷酸多态性(SNP)与语言特征缺陷之间的关联,该特征很好地表征了184个受特定语言障碍影响的家庭。结果:我们发现FOXP2结合并显着下调了CNTNAP2,CNTNAP2是一种编码神经毒素并在发育中的人类皮层中表达的基因。通过分析典型特殊语言障碍儿童的CNTNAP2多态性,我们检测到与无意义单词重复的显着定量关联,这是该疾病的可遗传行为标记(峰值关联,SNP rs17236239的P = 5.0x10(-5))。有趣的是,这一区域与自闭症儿童语言延迟有关。结论:FOXP2-CNTNAP2通路在涉及语言破坏的临床不同综合症之间提供了一种机制联系。

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