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在新皮层层内,突触后密度蛋白的进化受到不同功能约束。

Differential functional constraints on the evolution of postsynaptic density proteins in neocortical laminae.

机构信息

Department of Neuroscience, The University of Texas at Southwestern Medical Center, Dallas, Texas, United States of America.

出版信息

PLoS One. 2012;7(6):e39686. doi: 10.1371/journal.pone.0039686. Epub 2012 Jun 28.

Abstract

The postsynaptic density (PSD) is a protein dense complex on the postsynaptic membrane of excitatory synapses that is implicated in normal nervous system functions such as synaptic plasticity, and also contains an enrichment of proteins involved in neuropsychiatric disorders. It has recently been reported that the genes encoding PSD proteins evolved more slowly than other genes in the human brain, but the underlying evolutionary advantage for this is not clear. Here, we show that cortical gene expression levels could explain most of this effect, indicating that expression level is a primary contributor to the evolution of these genes in the brain. Furthermore, we identify a positive correlation between the expression of PSD genes and cortical layers, with PSD genes being more highly expressed in deep layers, likely as a result of layer-enriched transcription factors. As the cortical layers of the mammalian brain have distinct functions and anatomical projections, our results indicate that the emergence of the unique six-layered mammalian cortex may have provided differential functional constraints on the evolution of PSD genes. More superficial cortical layers contain PSD genes with less constraint and these layers are primarily involved in intracortical projections, connections that may be particularly important for evolved cognitive functions. Therefore, the differential expression and evolutionary constraint of PSD genes in neocortical laminae may be critical not only for neocortical architecture but the cognitive functions that are dependent on this structure.

摘要

突触后密度(PSD)是兴奋性突触后膜上的一种富含蛋白质的复合物,与正常神经系统功能有关,如突触可塑性,并且还包含丰富的与神经精神疾病相关的蛋白质。最近有报道称,编码 PSD 蛋白的基因在人类大脑中的进化速度比其他基因慢,但这种进化优势的潜在原因尚不清楚。在这里,我们表明皮质基因表达水平可以解释这种效应的大部分原因,表明表达水平是这些基因在大脑中进化的主要因素。此外,我们发现 PSD 基因的表达与皮质层之间存在正相关,PSD 基因在深层中表达更高,可能是由于层特异性转录因子的富集。由于哺乳动物大脑的皮质层具有独特的功能和解剖学投射,我们的结果表明,哺乳动物六层层状皮质的出现可能对 PSD 基因的进化提供了不同的功能限制。较浅的皮质层包含受限制较小的 PSD 基因,这些层主要参与皮质内投射,这些连接可能对进化认知功能尤为重要。因此,PSD 基因在新皮质层中的差异表达和进化限制不仅对新皮质结构而且对依赖于该结构的认知功能至关重要。

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