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一种用于感觉通路发育和可塑性的跨模态遗传框架。

A cross-modal genetic framework for the development and plasticity of sensory pathways.

机构信息

Department of Basic Neurosciences, University of Geneva, 1211 Geneva, Switzerland.

Clinic of Neurology, Geneva University Hospital, 1211 Geneva, Switzerland.

出版信息

Nature. 2016 Oct 6;538(7623):96-98. doi: 10.1038/nature19770. Epub 2016 Sep 26.

Abstract

Modality-specific sensory inputs from individual sense organs are processed in parallel in distinct areas of the neocortex. For each sensory modality, input follows a cortico-thalamo-cortical loop in which a 'first-order' exteroceptive thalamic nucleus sends peripheral input to the primary sensory cortex, which projects back to a 'higher order' thalamic nucleus that targets a secondary sensory cortex. This conserved circuit motif raises the possibility that shared genetic programs exist across sensory modalities. Here we report that, despite their association with distinct sensory modalities, first-order nuclei in mice are genetically homologous across somatosensory, visual, and auditory pathways, as are higher order nuclei. We further reveal peripheral input-dependent control over the transcriptional identity and connectivity of first-order nuclei by showing that input ablation leads to induction of higher-order-type transcriptional programs and rewiring of higher-order-directed descending cortical input to deprived first-order nuclei. These findings uncover an input-dependent genetic logic for the design and plasticity of sensory pathways, in which conserved developmental programs lead to conserved circuit motifs across sensory modalities.

摘要

个体感觉器官的特定感觉输入在新皮质的不同区域中平行处理。对于每种感觉模态,输入遵循皮质-丘脑-皮质回路,其中“一级”外感受丘脑核将外围输入发送到初级感觉皮层,该皮层再投射到靶向二级感觉皮层的“高级”丘脑核。这种保守的回路基序提出了这样一种可能性,即不同感觉模态之间存在共享的遗传程序。在这里,我们报告说,尽管与不同的感觉模态相关联,但小鼠中的一级核在躯体感觉、视觉和听觉通路上在遗传上是同源的,高级核也是如此。我们进一步揭示了外周输入对一级核的转录特性和连接性的依赖性控制,表明输入消融会导致高级类型转录程序的诱导以及剥夺一级核的高级定向下行皮质输入的重新布线。这些发现揭示了感觉通路的设计和可塑性的依赖于输入的遗传逻辑,其中保守的发育程序导致了不同感觉模态之间的保守回路基序。

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