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Neuronal-expressed microRNA-targeted pseudogenes compete with coding genes in the human brain

机译:神经元表达的靶向microRNA的假基因与人脑中的编码基因竞争

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摘要

MicroRNAs orchestrate brain functioning via interaction with microRNA recognition elements (MRE) on target transcripts. However, the global impact of potential competition on the microRNA pool between coding and non-coding brain transcripts that share MREs with them remains unexplored. Here we report that non-coding pseudogene transcripts carrying MREs (PSG+MRE) often show duplicated origin, evolutionary conservation and higher expression in human temporal lobe neurons than comparable duplicated MRE-deficient pseudogenes (PSG−MRE). PSG+MRE participate in neuronal RNA-induced silencing complexes (RISC), indicating functional involvement. Furthermore, downregulation cell culture experiments validated bidirectional co-regulation of PSG+MRE with MRE-sharing coding transcripts, frequently not their mother genes, and with targeted microRNAs; also, PSG+MRE single-nucleotide polymorphisms associated with schizophrenia, bipolar disorder and autism, suggesting interaction with mental diseases. Our findings indicate functional roles of duplicated PSG+MRE in brain development and cognition, supporting physiological impact of the reciprocal co-regulation of PSG+MRE with MRE-sharing coding transcripts in human brain neurons.
机译:MicroRNA通过与靶标转录物上的microRNA识别元件(MRE)相互作用来协调大脑功能。但是,潜在竞争对与它们共享MRE的编码和非编码大脑转录本之间的microRNA池的潜在影响尚待探索。在这里,我们报告携带MRE(PSG + MRE )的非编码假基因转录本与可比的重复MRE缺陷假基因(PSG )相比,在人颞叶神经元中通常显示出重复的起源,进化保守性和更高的表达。 -MRE )。 PSG + MRE 参与神经元RNA诱导的沉默复合物(RISC),表明其功能参与。此外,下调细胞培养实验验证了PSG + MRE 与MRE共享编码转录本(通常不是其母本基因)以及靶向微RNA的双向共调控。 PSG + MRE 单核苷酸多态性与精神分裂症,躁郁症和自闭症有关,提示与精神疾病的相互作用。我们的发现表明,重复的PSG + MRE 在大脑发育和认知中的功能作用,支持PSG + MRE 与MRE共享编码转录本相互相互调节的生理影响。人脑神经元。

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