Jan‐Marino Ramirez scite author profile

Observational studies in humans have found associations between overstimulation in infancy via excessive television viewing and subsequent deficits in cognition and attention. We developed and tested a mouse model of overstimulation whereby p10 mice were subjected to audio (70 db) and visual stimulation (flashing lights) for six hours per day for a total of 42 days. 10 days later cognition and behavior were tested using the following tests: Light Dark Latency, Elevated Plus Maze, Novel Object Recognition, and Barnes Maze. In all tests, overstimulated mice performed significantly worse compared to controls suggesting increased activity and risk taking, diminished short term memory, and decreased cognitive function. These findings suggest that excessive non-normative stimulation during critical periods of brain development can have demonstrable untoward effects on subsequent neurocognitive function.

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How early media exposure may affect cognitive function: A review of results from observations in humans and experiments in mice

Christakis

Ramirez

Ferguson

et al. 2018

Proc. Natl. Acad. Sci. U.S.A.

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Attention deficit hyperactivity disorder (ADHD) is now among the most commonly diagnosed chronic psychological dysfunctions of childhood. By varying estimates, it has increased by 30% in the past 20 years. Environmental factors that might explain this increase have been explored. One such factor may be audiovisual media exposure during early childhood. Observational studies in humans have linked exposure to fast-paced television in the first 3 years of life with subsequent attentional deficits in later childhood. Although longitudinal and well controlled, the observational nature of these studies precludes definitive conclusions regarding a causal relationship. As experimental studies in humans are neither ethical nor practical, mouse models of excessive sensory stimulation (ESS) during childhood, akin to the enrichment studies that have previously shown benefits of stimulation in rodents, have been developed. Experimental studies using this model have corroborated that ESS leads to cognitive and behavioral deficits, some of which may be potentially detrimental. Given the ubiquity of media during childhood, these findings in humansand rodents perhaps have important implications for public health.

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AUTS2 Regulates RNA Metabolism and Dentate Gyrus Development in Mice

Castanza

Ramirez²,

Tripathi³

et al. 2021

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Human AUTS2 mutations are linked to a syndrome of intellectual disability, autistic features, epilepsy, and other neurological and somatic disorders. Although it is known that this unique gene is highly expressed in developing cerebral cortex, the molecular and developmental functions of AUTS2 protein remain unclear. Using proteomics methods to identify AUTS2 binding partners in neonatal mouse cerebral cortex, we found that AUTS2 associates with multiple proteins that regulate RNA transcription, splicing, localization, and stability. Furthermore, AUTS2-containing protein complexes isolated from cortical tissue bound specific RNA transcripts in RNA immunoprecipitation and sequencing assays. Deletion of all major functional isoforms of AUTS2 (full-length and C-terminal) by conditional excision of exon 15 caused breathing abnormalities and neonatal lethality when Auts2 was inactivated throughout the developing brain. Mice with limited inactivation of Auts2 in cerebral cortex survived but displayed abnormalities of cerebral cortex structure and function, including dentate gyrus hypoplasia with agenesis of hilar mossy neurons, and abnormal spiking activity on EEG. Also, RNA transcripts that normally associate with AUTS2 were dysregulated in mutant mice. Together, these findings indicate that AUTS2 regulates RNA metabolism and is essential for development of cerebral cortex, as well as subcortical breathing centers.

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Intermittent Hypoxia Disrupts Adult Neurogenesis and Synaptic Plasticity in the Dentate Gyrus

Khuu

Pagan²,

Nallamothu

et al. 2018

J. Neurosci.

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CIH is an established model simulating the pattern of oxygenation experienced by individuals suffering from untreated sleep disordered breathing (SDB). In addition to the cardio‐respiratory effects, SDB has been shown to cause deficits in memory and learning. Previous studies conducted in CA1 neurons of the hippocampus indicate that CIH impairs synaptic plasticity in this neuronal population important to executive function. This ongoing study examines how CIH impacts the dentate gyrus (DG), another region of the hippocampus also important to memory and learning and known to exhibit neurogenesis throughout life. Histological analyses and electrophysiological experiments were conducted in the DG of mice (P60‐P80) exposed to CIH for 30 days. Although no difference in structural volume was observed within the hippocampal formation, the number of doublecortin positive cells found in the granular cell layer of the DG were fewer following CIH. Field recordings conducted in the DG of hippocampal brain slices revealed that CIH suppresses paired pulse facilitation at later interpulse intervals (200‐400ms). This significantly alters the paired pulse profile observed in control experiments. While CIH does not cause changes in gross structure of the DG, it results in altered neurogenesis and changed synaptic plasticity indicative of diffuse neuronal injury within an area central to executive function.

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