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Mammalian cortex features a vast diversity of neuronal cell types, each with characteristic anatomical, molecular and functional properties. Synaptic connectivity powerfully shapes how each cell type participates in the cortical circuit, but mapping connectivity rules at the resolution of distinct cell types remains difficult. Here, we used millimeter-scale volumetric electron microscopy1to investigate the connectivity of all inhibitory neurons across a densely-segmented neuronal population of 1352 cells spanning all layers of mouse visual cortex, producing a wiring diagram of inhibitory connections with more than 70,000 synapses. Taking a data-driven approach inspired by classical neuroanatomy, we classified inhibitory neurons based on the relative targeting of dendritic compartments and other inhibitory cells and developed a novel classification of excitatory neurons based on the morphological and synaptic input properties. The synaptic connectivity between inhibitory cells revealed a novel class of disinhibitory specialist targeting basket cells, in addition to familiar subclasses. Analysis of the inhibitory connectivity onto excitatory neurons found widespread specificity, with many interneurons exhibiting differential targeting of certain subpopulations spatially intermingled with other potential targets. Inhibitory targeting was organized into “motif groups,” diverse sets of cells that collectively target both perisomatic and dendritic compartments of the same excitatory targets. Collectively, our analysis identified new organizing principles for cortical inhibition and will serve as a foundation for linking modern multimodal neuronal atlases with the cortical wiring diagram.
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This content will become publicly available on June 25, 2026
A scalable, all-optical method for mapping synaptic connectivity with cell-type specificity
ABSTRACT Single-cell transcriptomics has uncovered the enormous heterogeneity of cell types that compose each region of the mammalian brain, but describing how such diverse types connect to form functional circuits has remained challenging. Current methods for measuring the probability and strength of cell-type specific connectivity motifs principally rely on low-throughput whole-cell recording approaches. The recent development of optical tools for perturbing and observing neural circuit activity, now notably including genetically encoded voltage indicators, presents an exciting opportunity to employ optical methods to greatly increase the throughput with which circuit connectivity can be mapped physiologically. At the same time, advances in spatial transcriptomics now enable the identification of cell typesin situbased on their unique gene expression signatures. Here, we demonstrate how long-range synaptic connectivity can be assayed optically with high sensitivity, high throughput, and cell-type specificity. We apply this approach in the motor cortex to examine cell-type-specific synaptic innervation patterns of long-range thalamic and contralateral input onto more than 1000 motor cortical neurons. We find that even cell types occupying the same cortical lamina receive vastly different levels of synaptic input, a finding which was previously not possible to uncover using lower-throughput approaches that can only describe the connectivity of broad cell types.
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- Award ID(s):
- 2215990
- PAR ID:
- 10654699
- Publisher / Repository:
- bioRxiv
- Date Published:
- Format(s):
- Medium: X
- Sponsoring Org:
- National Science Foundation
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