Abstract

Aberrant brain development during critical periods of heightened vulnerability contributes to lifelong cognitive impairments underlying many psychiatric disorders. Mechanisms driving critical period circuit development are well described in sensory systems-but poorly characterized for complex cognitive behaviors. Identification of a critical period and underlying mechanisms for cognitive circuits and behavior would eventually improve diagnosis, prevention and treatment of psychiatric disorders. This study will test whether a mechanism critical for regulating the critical period for visual cortex development also modulates maturation of frontal cortex- dependent attentional functions. Lynx1 is an endogenous nicotinic acetylcholine receptor (nAchR) inhibitor and regulates the critical period of visual cortex plasticity by its increased expression across adolescence. In addition to its role in visual cortex, our preliminary data show that the Lynx1 knock-out mice with high nAChR signaling unexpectedly present with attention-deficits in adulthood. Strikingly, this deficit was prevented by transient suppression of nAChR signaling only during early adolescence but not acutely in adulthood. This study will test the overarching hypothesis that the excessive nAChR signaling during adolescence, normally limited by peri-adolescent increase in Lynx1 expression, causes long-lasting impairment in frontal cortical circuits and behaviors that support attention. Understanding how excess nAChR signaling disrupts normal circuit development could provide mechanistic insight into developmental neuropsychiatric disorders characterized by disrupted nAChR signaling, such as Autism, ADHD and schizophrenia.
In Aim1, we will test the hypothesis that Lynx1 expression in anterior cingulate cortex during peri-adolescence is required for normal attentional function in the adult. We will precisely define the critical period and key brain regions mediating the long-lasting impact of excess nAChR signaling on adult attentional function by combining pharmacological, viral and genetic gene manipulations in vivo with 5-choice serial reaction time task (5- CCRTT) employing a translational touchscreen system.
In Aim2, we will test the hypothesis that the fronto- posterior cortical circuits require nAChR signaling to be suppressed by Lynx1 during adolescence to establish attention in the adult. By introducing a novel viral system that allows circuit-specific labeling and gene manipulations at time points of interest, the impact of Lynx1 deletion to neurons projecting from anterior cingulate cortex to visual cortex, and the cell-autonomous contribution of Lynx1 in these circuits will be determined. At the completion of this study, we will have defined the developmental time window, anatomical region, and circuit that require optimal nAChR signaling for normal attentional function, which is identified by the NIMH Research Domain Criteria (RDoC) project as one major construct of cognitive systems impaired in a number of psychiatric conditions.

Public Health Relevance

The goal of this study is to identify a developmental critical period and underlying mechanisms for establishing attentional circuits and behavior regulated by an endogenous inhibitor of nicotinic acetylcholine receptor called Lynx1. Such knowledge may represent a novel mechanism and therapeutic target for a cognitive function that is disturbed in developmental neuropsychiatric disorders including autism, ADHD, and schizophrenia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Mental Health (NIMH)
Type
Exploratory/Developmental Grants (R21)
Project #
1R21MH106919-01A1
Application #
9035003
Study Section
Developmental Brain Disorders Study Section (DBD)
Program Officer
Rossi, Andrew
Project Start
2015-12-16
Project End
2017-11-30
Budget Start
2015-12-16
Budget End
2016-11-30
Support Year
1
Fiscal Year
2016
Total Cost
$251,754
Indirect Cost
$101,754

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Psychiatry
Type
Schools of Medicine
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Smith, Milo R; Glicksberg, Benjamin S; Li, Li et al. (2018) Loss-of-function of neuroplasticity-related genes confers risk for human neurodevelopmental disorders. Pac Symp Biocomput 23:68-79
Smith, Milo R; Yevoo, Priscilla; Sadahiro, Masato et al. (2018) Integrative bioinformatics identifies postnatal lead (Pb) exposure disrupts developmental cortical plasticity. Sci Rep 8:16388
Morishita, Hirofumi; Arora, Manish (2017) Tooth-Matrix Biomarkers to Reconstruct Critical Periods of Brain Plasticity. Trends Neurosci 40:1-3
Steullet, P; Cabungcal, J-H; Coyle, J et al. (2017) Oxidative stress-driven parvalbumin interneuron impairment as a common mechanism in models of schizophrenia. Mol Psychiatry 22:936-943
Jiang, Yan; Loh, Yong-Hwee Eddie; Rajarajan, Prashanth et al. (2017) The methyltransferase SETDB1 regulates a large neuron-specific topological chromatin domain. Nat Genet 49:1239-1250
Lucas, Elizabeth K; Jegarl, Anita M; Morishita, Hirofumi et al. (2016) Multimodal and Site-Specific Plasticity of Amygdala Parvalbumin Interneurons after Fear Learning. Neuron 91:629-43
Sadahiro, Masato; Sajo, Mari; Morishita, Hirofumi (2016) Nicotinic regulation of experience-dependent plasticity in visual cortex. J Physiol Paris 110:29-36
Mitchell, Amanda C; Javidfar, Behnam; Bicks, Lucy K et al. (2016) Longitudinal assessment of neuronal 3D genomes in mouse prefrontal cortex. Nat Commun 7:12743
Smith, Milo R; Burman, Poromendro; Sadahiro, Masato et al. (2016) Integrative Analysis of Disease Signatures Shows Inflammation Disrupts Juvenile Experience-Dependent Cortical Plasticity. eNeuro 3:
Koike, Hiroyuki; Demars, Michael P; Short, Jennifer A et al. (2016) Chemogenetic Inactivation of Dorsal Anterior Cingulate Cortex Neurons Disrupts Attentional Behavior in Mouse. Neuropsychopharmacology 41:1014-23

Showing the most recent 10 out of 12 publications