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1. Nests of dividing neuroblasts sustain interneuron production for the developing human brain

   https://doi.org/10.1126/science.abk2346  

   Paredes, Mercedes F.; Mora, Cristina; Flores-Ramirez, Quetzal; Cebrian-Silla, Arantxa; Del Dosso, Ashley; Larimer, Phil; Chen, Jiapei; Kang, Gugene; Gonzalez Granero, Susana; Garcia, Eric; et al (January 2022, Science)

   INTRODUCTION Balance between excitatory and inhibitory neuron (interneuron) populations in the cortex promotes normal brain function. Interneurons are primarily generated in the medial, caudal, and lateral ganglionic eminences (MGE, CGE, and LGE) of the ventral embryonic forebrain; these subregions give rise to distinct interneuron subpopulations. In rodents, the MGE generates cortical interneurons, the parvalbumin + (PV + ) and somatostatin + (SST + ) subtypes that connect with excitatory neurons to regulate their activity. Defects in interneuron production have been implicated in neurodevelopmental and psychiatric disorders including autism, epilepsy, and schizophrenia. RATIONALE How does the human MGE (hMGE) produce the number of interneurons required to populate the forebrain? The hMGE contains progenitor clusters distinct from what has been observed in the rodent MGE and other germinal zones of the human brain. This cytoarchitecture could be the key to understanding interneuron neurogenesis. We investigated the cellular and molecular properties of different compartments within the developing hMGE, from 14 gestational weeks (GW) to 39 GW (term), to study their contribution to the production of inhibitory interneurons. We developed a xenotransplantation assay to follow the migration and maturation of the human interneurons derived from this germinal region. RESULTS Within the hMGE, densely packed aggregates (nests) of doublecortin + (DCX + ) and LHX6 + cells were surrounded by nestin + progenitor cells and their processes. These DCX + cell–enriched nests (DENs) were observed in the hMGE but not in the adjacent LGE. We found that cells within DENs expressed molecular markers associated with young neurons, such as DCX, and polysialylated neural cell adhesion molecule (PSA-NCAM). A subpopulation also expressed Ki-67, a marker of proliferation; therefore, we refer to these cells as neuroblasts. A fraction of DCX + cells inside DENs expressed SOX2 and E2F1, transcription factors associated with progenitor and proliferative properties. More than 20% of DCX + cells in the hMGE were dividing, specifically within DENs. Proliferating neuroblasts in DENs persisted in the hMGE throughout prenatal human brain development. The division of DCX + cells was confirmed by transmission electron microscopy and time-lapse microscopy. Electron microscopy revealed adhesion contacts between cells within DENs, providing multiple sites to anchor DEN cells together. Neuroblasts within DENs express PCDH19, and nestin + progenitors surrounding DENs express PCDH10; these findings suggest a role for differential cell adhesion in DEN formation and maintenance. When transplanted into the neonatal mouse brain, dissociated hMGE cells reformed DENs containing proliferative DCX + cells, similar to DENs observed in the prenatal human brain. This suggests that DENs are generated by cell-autonomous mechanisms. In addition to forming DENs, transplanted hMGE-derived neuroblasts generated young neurons that migrated extensively into cortical and subcortical regions in the host mouse brain. One year after transplantation, these neuroblasts had differentiated into distinct γ-aminobutyric acid–expressing (GABAergic) interneuron subtypes, including SST + and PV + cells, that showed morphological and functional maturation. CONCLUSION The hMGE harbors DENs, where cells expressing early neuronal markers continue to divide and produce GABAergic interneurons. This MGE-specific arrangement of neuroblasts in the human brain is present until birth, supporting expanded neurogenesis for inhibitory neurons. Given the robust neurogenic output from this region, knowledge of the mechanisms underlying cortical interneuron production in the hMGE will provide insights into the cell types and developmental periods that are most vulnerable to genetic or environmental insults. Nests of DCX + cells in the ventral prenatal brain. Schematic of a coronal view of the embryonic human forebrain showing the medial ganglionic eminence (MGE, green), with nests of DCX + cells (DENs, green). Nestin + progenitor cells (blue) are present within the VZ and iSVZ and are intercalated in the oSVZ (where DENs reside). The initial segment of the oSVZ contains palisades of nestin + progenitors referred to as type I clusters (light blue cells) around DENs. In the outer part of the oSVZ, DENs transition to chains of migrating DCX + cells; surrounding nestin + progenitors are arranged into groups of cells referred to as type II clusters (white cells). In addition to proliferation of nestin + progenitors, cell division is present among DCX + cells within DENs, suggesting multiple progenitor states for the generation of MGE-derived interneurons in the human forebrain. ILLUSTRATION: NOEL SIRIVANSANTI 

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2. Neuroanatomical Alterations in the CNTNAP2 Mouse Model of Autism Spectrum Disorder

   https://doi.org/10.3390/brainsci13060891  

   Gandhi, Tanya; Canepa, Cade R; Adeyelu, Tolulope T; Adeniyi, Philip A; Lee, Charles C (June 2023, Brain Sciences)

   Autism spectrum disorder (ASD) is associated with neurodevelopmental alterations, including atypical forebrain cellular organization. Mutations in several ASD-related genes often result in cerebral cortical anomalies, such as the abnormal developmental migration of excitatory pyramidal cells and the malformation of inhibitory neuronal circuitry. Notably here, mutations in the CNTNAP2 gene result in ectopic superficial cortical neurons stalled in lower cortical layers and alterations to the balance of cortical excitation and inhibition. However, the broader circuit-level implications of these findings have not been previously investigated. Therefore, we assessed whether ectopic cortical neurons in CNTNAP2 mutant mice form aberrant connections with higher-order thalamic nuclei, potentially accounting for some autistic behaviors, such as repetitive and hyperactive behaviors. Furthermore, we assessed whether the development of parvalbumin-positive (PV) cortical interneurons and their specialized matrix support structures, called perineuronal nets (PNNs), were altered in these mutant mice. We found alterations in both ectopic neuronal connectivity and in the development of PNNs, PV neurons and PNNs enwrapping PV neurons in various sensory cortical regions and at different postnatal ages in the CNTNAP2 mutant mice, which likely lead to some of the cortical excitation/inhibition (E/I) imbalance associated with ASD. These findings suggest neuroanatomical alterations in cortical regions that underlie the emergence of ASD-related behaviors in this mouse model of the disorder. 

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3. Parvalbumin neurons enhance temporal coding and reduce cortical noise in complex auditory scenes

   https://doi.org/10.1038/s42003-023-05126-0  

   Nocon, Jian_Carlo; Gritton, Howard_J; James, Nicholas_M; Mount, Rebecca_A; Qu, Zhili; Han, Xue; Sen, Kamal (July 2023, Communications Biology)

   Abstract Cortical representations supporting many cognitive abilities emerge from underlying circuits comprised of several different cell types. However, cell type-specific contributions to rate and timing-based cortical coding are not well-understood. Here, we investigated the role of parvalbumin neurons in cortical complex scene analysis. Many complex scenes contain sensory stimuli which are highly dynamic in time and compete with stimuli at other spatial locations. Parvalbumin neurons play a fundamental role in balancing excitation and inhibition in cortex and sculpting cortical temporal dynamics; yet their specific role in encoding complex scenes via timing-based coding, and the robustness of temporal representations to spatial competition, has not been investigated. Here, we address these questions in auditory cortex of mice using a cocktail party-like paradigm, integrating electrophysiology, optogenetic manipulations, and a family of spike-distance metrics, to dissect parvalbumin neurons’ contributions towards rate and timing-based coding. We find that suppressing parvalbumin neurons degrades cortical discrimination of dynamic sounds in a cocktail party-like setting via changes in rapid temporal modulations in rate and spike timing, and over a wide range of time-scales. Our findings suggest that parvalbumin neurons play a critical role in enhancing cortical temporal coding and reducing cortical noise, thereby improving representations of dynamic stimuli in complex scenes. 

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4. Ectopic brain-derived insulin-like growth factor-1 partially rescues neuroanatomical defects associated with developmental hypothyroidism

   Alexandra, Grond; Saatman, Kathryn; Sharlin, David S. (November 2018, Abstracts - Society for Neuroscience)

   Insufficient thyroid hormone (TH) during development results in permanent neurological deficits. These deficits are the result of neuroanatomical defects that include smaller brain, fewer parvalbumin neurons, and hypomyelination. Interestingly, insufficient insulin-like growth factor 1 (Igf-1) during development results in similar neuroanatomical defects to those reported for developmental hypothyroidism. Thyroid hormone is known to indirectly influence serum Igf-1 levels through its regulation of pituitary growth hormone (GH) secretion which stimulates hepatic Igf-1 production. Our lab and others have observed decreases of local brain-derived Igf-1 in the developing hypothyroid mouse brain. This observation suggests that deficits associated with low TH during development may be the result of altered brain-derived Igf-1. Considering this, we sought to determine whether ectopically expressing Igf-1 in the developing brain could rescue neuroanatomical defects associated with TH. To accomplish this, the tet-off transgenic system was used where mice harboring tetracycline transactivator protein driven by the human GFAP promoter (tTA-GFAP) were crossed with mice containing the human Igf-1cDNA under the control the TET response element (Igf1-pTRE) transgene. Double transgenic (dTg) offspring carrying both the tTA-GFAP and Igf1-TRE genes overexpress Igf-1 specifically in brain astrocytes. The timed-pregnant mice were treated with thyroid gland inhibitors from embryonic day 14.5 (E14.5) until postnatal day 14 (P14) to induce a hypothyroid state in pups. At P14, pups were weighed and sacrificed, trunk blood was collected, and brains were dissected, weighed, and immediately frozen. Hippocampal structure, known be disrupted by developmental hypothyroidism, was assessed by fluorescent imaging using DAPI staining. Our initial results indicate that ectopic expression of Igf-1 in the brain (dTg mice) rescues hypothyroidism-induced reductions in brain weight without increasing body weight. In addition, the ectopic expression of Igf-1 restored hypothyroidism-induced perturbations in dentate gyrus size. Ongoing studies are using quantitative real-time PCR on micro-dissected cortical and hippocampal samples, to quantify myelin associated glycoprotein and parvalbumin mRNAs. Taken together, our findings support the idea that ectopic brain-derived Igf-1 rescues neuroanatomical defects caused by hypothyroidism and implicates TH in the regulation of brain Igf-1. 

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5. Fine Control of Sound Frequency Tuning and Frequency Discrimination Acuity by Synaptic Zinc Signaling in Mouse Auditory Cortex

   https://doi.org/10.1523/JNEUROSCI.1339-18.2018  

   Kumar, Manoj; Xiong, Shanshan; Tzounopoulos, Thanos; Anderson, Charles T. (January 2019, The Journal of Neuroscience)

   Neurons in the auditory cortex are tuned to specific ranges of sound frequencies. Although the cellular and network mechanisms underlying neuronal sound frequency selectivity are well studied and reflect the interplay of thalamocortical and intracortical excitatory inputs and further refinement by cortical inhibition, the precise synaptic signaling mechanisms remain less understood. To gain further understanding on these mechanisms and their effects on sound-driven behavior, we used in vivo imaging as well as behavioral approaches in awake and behaving female and male mice. We discovered that synaptic zinc, a modulator of neurotransmission and responsiveness to sound, sharpened the sound frequency tuning of principal and parvalbumin-expressing neurons and widened the sound frequency tuning of somatostatin-expressing inhibitory neurons in layer 2/3 of the primary auditory cortex. In the absence of cortical synaptic zinc, mice exhibited reduced acuity for detecting changes in sound frequencies. Together, our results reveal that cell-type-specific effects of zinc contribute to cortical sound frequency tuning and enhance acuity for sound frequency discrimination. SIGNIFICANCE STATEMENT Neuronal tuning to specific features of sensory stimuli is a fundamental property of cortical sensory processing that advantageously supports behavior. Despite the established roles of synaptic thalamocortical and intracortical excitation and inhibition in cortical tuning, the precise synaptic signaling mechanisms remain unknown. Here, we investigated these mechanisms in the mouse auditory cortex. We discovered a previously unknown signaling mechanism linking synaptic zinc signaling with cell-specific cortical tuning and enhancement in sound frequency discrimination acuity. Given the abundance of synaptic zinc in all sensory cortices, this newly discovered interaction between synaptic zinc and cortical tuning can provide a general mechanism for modulating neuronal stimulus specificity and sensory-driven behavior. 

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