Abstract

A general theory of neural development holds that sensory experience can influence the functional properties of synapses during a finite period of maturation (i.e., critical period). Consistent with this idea, cortical inhibitory synapse strength is reduced dramatically following even moderate developmental hearing loss. However, whether inhibitory synapse maturation displays a critical period is poorly understood. Further, there are no strategies to restore normal inhibitory function in animals raised with hearing loss. Our core hypothesis is that cortical inhibitory synapse function is particularly vulnerable to hearing loss before adulthood, and normal function can be rescued during a critical period. There are three related aims:
Aim 1 will first determine whether the effect of developmental conductive hearing loss (CHL) on auditory cortex inhibitory synapse function persists into adulthood. We will then ask whether inhibitory function in auditory cortex is more vulnerable to CHL that occurs during early development, than to CHL that occurs in late juvenile or adult animals. In all cases, spontaneous and evoked inhibitory synaptic currents will be recorded in a thalamocortical brain slice, including paired recordings between inhibitory interneurons and pyramidal cells.
Aim 2 will determine whether inhibitory synapse deficits induced by developmental CHL can impair auditory processing. Using a large-scale auditory cortex network model that incorporates parameters based on in situ measurements, we will evaluate how specific inhibitory properties influence the simulations of auditory cortex coding. Comparisons will be made between 'control'networks and 'CHL networks'in which one or more inhibitory property is modified to reflect experimental observations.
Aim 3 will determine whether normal inhibitory function can be permanently rescued in animals with developmental CHL by rearing them with a GABAergic agonist for 6 days. Animals will then be permitted to reach adulthood, when inhibitory synaptic properties will be assessed. The agonists to be used will activate either 11 subunit-containing GABAA receptors, or GABAA and GABAB receptors or GABAB receptors only. To determine whether there is a critical period during which inhibitory function can be rescued, animals with early CHL will be drug-treated later during juvenile development or as adults. Finally, if we find that adult CHL produces inhibitory synaptic dysfunction, then we will determine whether drug-rearing can rescue inhibition in these animals. Together, these data will provide the first analysis of an inhibitory synapse critical period in the auditory system, and a first attempt to pharmacologically rescue central nervous system function following developmental hearing loss.

Public Health Relevance

Profound hearing loss in children can produce long-lasting deficits in auditory perception and language acquisition. It has been suggested that central nervous system deficits that are caused by hearing loss could adversely impact auditory processing and perception. Therefore, restoration of central function could be essential for the development of normal auditory performance. To address this issue, we will explore whether auditory cortex synapse function is particularly vulnerable to hearing loss, and evaluate a new strategy for restoring normal synapse function in animals with developmental hearing loss.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Project (R01)
Project #
5R01DC011284-04
Application #
8579798
Study Section
Auditory System Study Section (AUD)
Program Officer
Platt, Christopher
Project Start
2010-12-10
Project End
2015-11-30
Budget Start
2013-12-01
Budget End
2014-11-30
Support Year
4
Fiscal Year
2014
Total Cost
$462,716
Indirect Cost
$160,712

  Institution

Name
New York University
Department
Neurology
Type
Schools of Arts and Sciences
DUNS #
041968306
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Zorio, Diego A R; Monsma, Scott; Sanes, Dan H et al. (2018) De novo sequencing and initial annotation of the Mongolian gerbil (Meriones unguiculatus) genome. Genomics :
Kotak, Vibhakar C; Mirallave, Ana; Mowery, Todd M et al. (2017) GABAergic inhibition gates excitatory LTP in perirhinal cortex. Hippocampus 27:1217-1223
Mowery, Todd M; Penikis, Kristina B; Young, Stephen K et al. (2017) The Sensory Striatum Is Permanently Impaired by Transient Developmental Deprivation. Cell Rep 19:2462-2468
Dimidschstein, Jordane; Chen, Qian; Tremblay, Robin et al. (2016) A viral strategy for targeting and manipulating interneurons across vertebrate species. Nat Neurosci 19:1743-1749
Mowery, Todd M; Kotak, Vibhakar C; Sanes, Dan H (2016) The onset of visual experience gates auditory cortex critical periods. Nat Commun 7:10416
Sarro, Emma C; von Trapp, Gardiner; Mowery, Todd M et al. (2015) Cortical Synaptic Inhibition Declines during Auditory Learning. J Neurosci 35:6318-25
Kotak, Vibhakar C; Mowery, Todd M; Sanes, Dan H (2015) Characterization of auditory synaptic inputs to gerbil perirhinal cortex. Front Neural Circuits 9:40
Mowery, Todd M; Kotak, Vibhakar C; Sanes, Dan H (2015) Transient Hearing Loss Within a Critical Period Causes Persistent Changes to Cellular Properties in Adult Auditory Cortex. Cereb Cortex 25:2083-94
Gai, Yan; Kotak, Vibhakar C; Sanes, Dan H et al. (2014) On the localization of complex sounds: temporal encoding based on input-slope coincidence detection of envelopes. J Neurophysiol 112:802-13
Takesian, Anne E; Kotak, Vibhakar C; Sharma, Neeti et al. (2013) Hearing loss differentially affects thalamic drive to two cortical interneuron subtypes. J Neurophysiol 110:999-1008

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