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    Date Issued2022 (1)2021 (2)Author
    Faust, Travis E. (3)
    Schafer, Dorothy P (3)Andrews, Gregory (1)Baer, Christina E. (1)Donnard, Elisa (1)View MoreUMass Chan AffiliationNeurobiology (3)Schafer Lab (3)Brudnick Neuropsychiatric Research Institute (1)Graduate School of Biomedical Sciences, Neuroscience Program (1)Microbiology and Physiological Systems (1)View MoreDocument TypeJournal Article (3)KeywordDevelopmental Neuroscience (2)Molecular and Cellular Neuroscience (2)Amino Acids, Peptides, and Proteins (1)Cellular neuroscience (1)Immunity (1)View MoreJournalImmunity (1)Nature neuroscience (1)Nature reviews. Neuroscience (1)

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    Spatial transcriptomic reconstruction of the mouse olfactory glomerular map suggests principles of odor processing

    Wang, I-Hao; Andrews, Gregory; Donnard, Elisa; Duran-Laforet, Violeta; Faust, Travis E.; Garber, Manuel; Baer, Christina E.; Schafer, Dorothy P; Weng, Zhiping; Greer, Paul L. (2022-03-21)
    The olfactory system's ability to detect and discriminate between the vast array of chemicals present in the environment is critical for an animal's survival. In mammals, the first step of this odor processing is executed by olfactory sensory neurons, which project their axons to a stereotyped location in the olfactory bulb (OB) to form glomeruli. The stereotyped positioning of glomeruli in the OB suggests an importance for this organization in odor perception. However, because the location of only a limited subset of glomeruli has been determined, it has been challenging to determine the relationship between glomerular location and odor discrimination. Using a combination of single-cell RNA sequencing, spatial transcriptomics and machine learning, we have generated a map of most glomerular positions in the mouse OB. These observations significantly extend earlier studies and suggest an overall organizational principle in the OB that may be used by the brain to assist in odor decoding.
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    IL-6 boosts synaptogenesis STAT!

    Faust, Travis E.; Schafer, Dorothy P (2021-11-09)
    Maternal infection during pregnancy increases the offspring's risk of developing neurodevelopmental disorders. While IL-6 is involved, the mechanism by which IL-6 and other cytokines affect developing neural circuits is unknown. In this issue of Immunity, Mirabella et al. (2021) show that the pro-inflammatory cytokine IL-6 specifically increases synaptogenesis in immature excitatory neurons through downstream neuronal STAT3-dependent transcriptional regulation of Rgs4.
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    Mechanisms governing activity-dependent synaptic pruning in the developing mammalian CNS

    Faust, Travis E.; Gunner, Georgia; Schafer, Dorothy P (2021-11-01)
    Almost 60 years have passed since the initial discovery by Hubel and Wiesel that changes in neuronal activity can elicit developmental rewiring of the central nervous system (CNS). Over this period, we have gained a more comprehensive picture of how both spontaneous neural activity and sensory experience-induced changes in neuronal activity guide CNS circuit development. Here we review activity-dependent synaptic pruning in the mammalian CNS, which we define as the removal of a subset of synapses, while others are maintained, in response to changes in neural activity in the developing nervous system. We discuss the mounting evidence that immune and cell-death molecules are important mechanistic links by which changes in neural activity guide the pruning of specific synapses, emphasizing the role of glial cells in this process. Finally, we discuss how these developmental pruning programmes may go awry in neurodevelopmental disorders of the human CNS, focusing on autism spectrum disorder and schizophrenia. Together, our aim is to give an overview of how the field of activity-dependent pruning research has evolved, led to exciting new questions and guided the identification of new, therapeutically relevant mechanisms that result in aberrant circuit development in neurodevelopmental disorders.
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