Beyond barrels: diverse thalamocortical projection motifs in the mouse ventral posterior complex

神经科学 投影(关系代数) 生物 解剖 人工智能 计算机科学 算法
作者
Mario Rubio-Teves,Pablo J. Martin-Correa,Carmen Alonso-Martínez,Diana Casas-Torremocha,María García‐Amado,Nestor Timonidis,Francesco Jamal Sheiban,Rembrandt Bakker,Paul Tiesinga,César Porrero,Francisco Clascá
出处
期刊:The Journal of Neuroscience [Society for Neuroscience]
卷期号:: e1096242024-e1096242024
标识
DOI:10.1523/jneurosci.1096-24.2024
摘要

Thalamocortical pathways from the rodent ventral posterior (VP) thalamic complex to the somatosensory cerebral cortex areas are a key model in modern neuroscience. However, beyond the intensively-studied projection from medial VP (VPM) to the primary somatosensory area (S1), the wiring of these pathways remains poorly characterized. We combined micropopulation tract-tracing and single-cell transfection experiments to map the pathways arising from different portions of the ventral posterior complex (VP) in male mice. We found that pathways originating from different VP regions show differences in area/lamina arborization pattern and axonal varicosity size. Neurons from the rostral VPM subnucleus innervate trigeminal S1 in point-to-point fashion. In contrast, a caudal VPM subnucleus innervates heavily and topographically S2, but not S1. Neurons in a third, intermediate VPM subnucleus innervate through branched axons both S1 and S2, with markedly different laminar patterns in each area. A small anterodorsal subnucleus selectively innervates dysgranular S1. The parvicellular VP subnucleus selectively targets the insular cortex, and adjacent portions of S1 and S2. Neurons in the rostral part of the lateral VP nucleus (VPL) innervate spinal S1, while caudal VPL neurons simultaneously target S1 and S2. Rostral and caudal VP nuclei show complementary patterns of calcium-binding protein expression. In addition to cortex, neurons in caudal VP subnuclei target the sensorimotor striatum. Our finding of a massive projection from VP to S2 separate from the VP projections to S1 adds critical anatomical evidence to the notion that different somatosensory submodalities are processed in parallel in S1 and S2.

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