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Human visual cortex is organized along two genetically opposed hierarchical gradients with unique developmental and evolutionary origins

机译:人类视觉皮层是沿着两个具有独特的发育和进化起源的遗传对立的层次梯度组织的

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摘要

Human visual cortex is organized with striking consistency across individuals. While recent findings demonstrate an unexpected coupling between functional and cytoarchitectonic regions relative to the folding of human visual cortex, a unifying principle linking these anatomical and functional features of the cortex remains elusive. To fill this gap in knowledge, we combined independent and ground truth measurements of cytoarchitectonic regions and genetic tissue characterization within human occipitotemporal cortex. Using a data-driven approach, we examined whether differential gene expression among cytoarchitectonic areas could contribute to the arealization of occipitotemporal cortex into a hierarchy based on transcriptomics. This approach revealed two opposing gene expression gradients: one that contains a series of genes with expression magnitudes that ascend from posterior (e.g., areas human occipital [hOc]1, hOc2, hOc3, etc.) to anterior cytoarchitectonic areas (e.g., areas fusiform gyrus [FG]1–FG4) and another that contains a separate series of genes that show a descending gradient from posterior to anterior areas. Using data from the living human brain, we show that each of these gradients correlates strongly with variations in measures related to either thickness or myelination of cortex, respectively. We further reveal that these genetic gradients emerge along unique trajectories in human development: the ascending gradient is present at 10–12 gestational weeks, while the descending gradient emerges later (19–24 gestational weeks). Interestingly, it is not until early childhood (before 5 years of age) that the two expression gradients achieve their adult-like mean expression values. Additional analyses in nonhuman primates (NHPs) reveal that homologous genes do not generate the same ascending and descending expression gradients as in humans. We discuss these findings relative to previously proposed hierarchies based on functional and cytoarchitectonic features of visual cortex. Altogether, these findings bridge macroscopic features of human cytoarchitectonic areas in visual cortex with microscopic features of cellular organization and genetic expression, which, despite the complexity of this multiscale correspondence, can be described by a sparse subset (approximately 200) of genes. These findings help pinpoint the genes contributing to healthy cortical development and explicate the cortical biology distinguishing humans from other primates, as well as establishing essential groundwork for understanding future work linking genetic mutations with the function and development of the human brain.
机译:人类视觉皮层的组织结构具有惊人的一致性。尽管最近的发现表明功能区和细胞结构区之间相对于人类视觉皮层的折叠是出乎意料的耦合,但是将皮层的这些解剖和功能特征联系起来的统一原理仍然难以捉摸。为了填补这一知识空白,我们结合了细胞枕区域的独立和地面真实测量以及人类枕颞皮层内的遗传组织表征。使用数据驱动的方法,我们检查了细胞建筑区域之间的差异基因表达是否可能有助于枕叶皮质区域化成基于转录组学的层次结构。这种方法揭示了两个相反的基因表达梯度:一个包含一系列表达幅度从后部(例如人枕[hOc] 1,hOc2,hOc3等)到前细胞建筑区域(例如梭形区域)的基因。 gyrus [FG] 1-FG4)和另一个包含一系列独立基因的序列,这些基因显示从后到前的递减梯度。使用来自活人脑的数据,我们显示这些梯度中的每一个都分别与皮质的厚度或髓鞘化相关的量度变化密切相关。我们进一步揭示了这些遗传梯度沿着人类发展的独特轨迹出现:上升梯度出现在10至12个孕周,而下降梯度出现于较晚(19-24个孕周)。有趣的是,直到儿童早期(5岁之前),这两个表达梯度才达到其成年人般的平均表达值。在非人类灵长类动物(NHP)中进行的其他分析表明,同源基因不会产生与人类相同的上升和下降表达梯度。我们讨论这些发现相对于以前提出的基于视觉皮层的功能和细胞结构特征的层次结构。总而言之,这些发现桥接了视觉皮层中人类细胞建筑区域的宏观特征与细胞组织和遗传表达的微观特征,尽管这种多尺度对应关系很复杂,但可以用基因的稀疏子集(约200个)来描述。这些发现有助于查明有助于健康皮质发育的基因,并阐明使人类与其他灵长类动物区分开的皮质生物学,以及为理解将遗传突变与人脑功能和发育联系起来的未来工作奠定基础。

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