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Mir-132/212 is required for maturation of binocular matching of orientation preference and depth perception

机译:Mir-132 / 212是定向取向和深度感知的双目匹配成熟所必需的

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摘要

MicroRNAs (miRNAs) are known to mediate post-transcriptional gene regulation, but their role in postnatal brain development is still poorly explored. We show that the expression of many miRNAs is dramatically regulated during functional maturation of the mouse visual cortex with miR-132/212 family being one of the top upregulated miRNAs. Age-downregulated transcripts are significantly enriched in miR-132/miR-212 putative targets and in genes upregulated in miR-132/212 null mice. At a functional level, miR-132/212 deletion affects development of receptive fields of cortical neurons determining a specific impairment of binocular matching of orientation preference, but leaving orientation and direction selectivity unaltered. This deficit is associated with reduced depth perception in the visual cliff test. Deletion of miR-132/212 from forebrain excitatory neurons replicates the binocular matching deficits. Thus, miR-132/212 family shapes the age-dependent transcriptome of the visual cortex during a specific developmental window resulting in maturation of binocular cortical cells and depth perception.
机译:已知MicroRNA(miRNA)介导转录后的基因调控,但在产后大脑发育中的作用仍未得到很好的研究。我们显示,在小鼠视觉皮层功能成熟期间,miR-132 / 212家族是最上调的miRNA之一,许多miRNA的表达受到了显着调节。年龄下调的转录本在miR-132 / miR-212推定的靶标和在miR-132 / 212无效小鼠中上调的基因中明显丰富。在功能水平上,miR-132 / 212缺失会影响皮质神经元感受野的发育,从而决定了定向偏好的双目匹配的特定损伤,但定向和方向选择性保持不变。这种缺陷与视觉悬崖测试中深度感知的减少有关。从前脑兴奋性神经元中删除miR-132 / 212复制了双眼匹配缺陷。因此,miR-132 / 212家族在特定的发育窗口期间塑造了视皮层的年龄依赖性转录组,导致双眼皮层细胞成熟和深度感知。

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