Publications by authors named "Sergiy Popovych"

Article Synopsis
  • Researchers have created a detailed neuronal wiring diagram of the whole brain of a fruit fly (Drosophila melanogaster), mapping over 5 billion chemical synapses between more than 139,000 neurons, to better understand brain function.
  • The study includes detailed annotations about various cell types, nerve pathways, and neurotransmitter identities, and the data is freely available for other researchers to use and explore.
  • By analyzing synaptic pathways and connections, the project helps illustrate how neural structures relate to sensorimotor behaviors, paving the way for similar studies in other species.
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The reconstruction of neural circuits from serial section electron microscopy (ssEM) images is being accelerated by automatic image segmentation methods. Segmentation accuracy is often limited by the preceding step of aligning 2D section images to create a 3D image stack. Precise and robust alignment in the presence of image artifacts is challenging, especially as datasets are attaining the petascale.

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Advances in Electron Microscopy, image segmentation and computational infrastructure have given rise to large-scale and richly annotated connectomic datasets which are increasingly shared across communities. To enable collaboration, users need to be able to concurrently create new annotations and correct errors in the automated segmentation by proofreading. In large datasets, every proofreading edit relabels cell identities of millions of voxels and thousands of annotations like synapses.

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Connections between neurons can be mapped by acquiring and analyzing electron microscopic (EM) brain images. In recent years, this approach has been applied to chunks of brains to reconstruct local connectivity maps that are highly informative, yet inadequate for understanding brain function more globally. Here, we present the first neuronal wiring diagram of a whole adult brain, containing 5×10 chemical synapses between ~130,000 neurons reconstructed from a female .

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Article Synopsis
  • Understanding how circuit connectivity influences brain function is key to grasping brain computations, especially in the mouse primary visual cortex (V1), where similar-response neurons tend to be synaptically linked.
  • This study used a large dataset to show that neuronal connections are based not only within V1 but also span across different cortical layers and areas, indicating a 'like-to-like' connectivity rule throughout the visual system.
  • Additionally, a digital model revealed that neuronal response features, rather than their physical location, primarily predict synaptic connections, suggesting both basic and complex connectivity patterns that impact sensory processing and learning in both biological and artificial neural networks.
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We are now in the era of millimeter-scale electron microscopy (EM) volumes collected at nanometer resolution. Dense reconstruction of cellular compartments in these EM volumes has been enabled by recent advances in Machine Learning (ML). Automated segmentation methods produce exceptionally accurate reconstructions of cells, but post-hoc proofreading is still required to generate large connectomes free of merge and split errors.

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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 microscopy to 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.

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Neurons in the developing brain undergo extensive structural refinement as nascent circuits adopt their mature form. This physical transformation of neurons is facilitated by the engulfment and degradation of axonal branches and synapses by surrounding glial cells, including microglia and astrocytes. However, the small size of phagocytic organelles and the complex, highly ramified morphology of glia have made it difficult to define the contribution of these and other glial cell types to this crucial process.

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Learning from experience depends at least in part on changes in neuronal connections. We present the largest map of connectivity to date between cortical neurons of a defined type (layer 2/3 [L2/3] pyramidal cells in mouse primary visual cortex), which was enabled by automated analysis of serial section electron microscopy images with improved handling of image defects (250 × 140 × 90 μm volume). We used the map to identify constraints on the learning algorithms employed by the cortex.

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Article Synopsis
  • A semi-automated reconstruction of the L2/3 region of the mouse primary visual cortex was created using electron microscopy images, capturing various cell types and structures important for understanding visual processing.
  • The data includes visual response characteristics of pyramidal cells and is available for public access, along with interactive tools for analysis.
  • Research highlights how the organization of mitochondria and synapses relates to cell location, while predicting connectivity patterns in pyramidal cells correlates with their visual response strength and reliability.
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Article Synopsis
  • Advances in automated imaging now allow for the mapping of entire brains, with projects needing significant time for data proofreading due to their size.
  • FlyWire is introduced as an online platform that enables collaborative proofreading of neural circuits in fruit flies, utilizing 3D interactive tools for efficient editing from anywhere.
  • The platform encourages community participation, enhances data accuracy, and promotes faster scientific discoveries, showcased through the analysis of mechanosensory neurons' connectome.
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Inhibitory neurons in mammalian cortex exhibit diverse physiological, morphological, molecular, and connectivity signatures. While considerable work has measured the average connectivity of several interneuron classes, there remains a fundamental lack of understanding of the connectivity distribution of distinct inhibitory cell types with synaptic resolution, how it relates to properties of target cells, and how it affects function. Here, we used large-scale electron microscopy and functional imaging to address these questions for chandelier cells in layer 2/3 of the mouse visual cortex.

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