Abstract

The goal of this second revised application is to investigate the ontogenetic mechanisms that underlie cholinergic synaptogenesis in the inner ear. Although synapse formation is best understood at the neuromuscular junction (NMJ), the applicability of this cholinergic model to other synapses in the nervous system has proved difficult. We propose to investigate cholinergic synapse formation, maturation and maintenance using vital, molecular and immunocytochemical methods in normal and transgenic animals as well as in organotypic culture. Specifically, we will explore the spatiotemporal expression, acquisition and loss of nicotinic receptors (formation), the localization of receptor clusters to cholinergic synapses (differentiation), and how these postsynaptic receptor clusters are maintained. Our basic hypothesis that bi-directional signaling between hair cells and efferent nerve terminals regulates the formation, differentiation and maintenance of cholinergic synapses, will be tested.
Specific aim 1 investigates the hypothesis that the formation of nicotinic acetylcholine receptors (nAChRs) is independent of efferent innervation. Using embryonic mutant animals and organotypic culture explants from embryonic inner ears, we will characterize the expression and formation of nAChRs in the absence of cholinergic input. We will characterize the relation between the differential expression of nAChR subunits, the development of nAChR clusters, and efferent innervation. We will identify the time of appearance, cellular distribution, and degree of co-localization between nAChRs and presynaptic cholinergic terminals. We will also investigate the formation of nAChRs in vestibular hair cells.
Specific aim 2 investigates the hypothesis that the differentiation of postsynaptic nicotinic receptors depends on cholinergic innervation. In postnatal animals, we will determine if nAChRs colocalize with medial or lateral olivocochlear neurons and the extent of colocalization between nAChR clusters and cholinergic innervation. We will investigate whether postsynaptic differentiation occurs after a loss of cholinergic input.
Specific aim 3 investigates the hypothesis that the maintenance of postsynaptic nAChR clusters is dependent on medial efferent innervation. In mature and postnatal animals, we will characterize the loss of nAChR expression and clusters after elimination of cholinergic input.
Specific aim 4 investigates the hypothesis that nAChR clustering in hair cells involves similar signaling molecules as found at the NMJ. We will investigate nAChR expression and clustering in transgenic mutant models that lack agrin, rapsyn or MuSK, all shown to be key factors in clustering at the NMJ. We will also characterize interactions between the hair cell nAChRs and these NMJ signaling molecules. In summary, these studies of cholinergic synapse development in the inner ear should have broad implications for the study of synapse formation throughout the nervous system as well as for a range of specific disorders associated defective cholinergic neurotransmission.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Deafness and Other Communication Disorders (NIDCD)
Type
Research Project (R01)
Project #
5R01DC004086-08
Application #
6987175
Study Section
Auditory System Study Section (AUD)
Program Officer
Freeman, Nancy
Project Start
1998-08-01
Project End
2009-11-30
Budget Start
2005-12-01
Budget End
2006-11-30
Support Year
8
Fiscal Year
2006
Total Cost
$375,044
Indirect Cost

  Institution

Name
Washington University
Department
Otolaryngology
Type
Schools of Medicine
DUNS #
068552207
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Hoffman, Larry F; Choy, Kristel R; Sultemeier, David R et al. (2018) Oncomodulin Expression Reveals New Insights into the Cellular Organization of the Murine Utricle Striola. J Assoc Res Otolaryngol 19:33-51
Tong, Benton; Hornak, Aubrey J; Maison, Stéphane F et al. (2016) Oncomodulin, an EF-Hand Ca2+ Buffer, Is Critical for Maintaining Cochlear Function in Mice. J Neurosci 36:1631-5
Simmons, Dwayne D; Lohr, Rachel; Wotring, Helena et al. (2014) Recovery of otoacoustic emissions after high-level noise exposure in the American bullfrog. J Exp Biol 217:1626-36
Miller, Mia E; Nasiri, Arian K; Farhangi, Peyman O et al. (2012) Evidence for water-permeable channels in auditory hair cells in the leopard frog. Hear Res 292:64-70
Arch, Victoria S; Simmons, Dwayne D; Quiñones, Patricia M et al. (2012) Inner ear morphological correlates of ultrasonic hearing in frogs. Hear Res 283:70-9
Simmons, D D; Morley, B J (2011) Spatial and temporal expression patterns of nicotinic acetylcholine ?9 and ?10 subunits in the embryonic and early postnatal inner ear. Neuroscience 194:326-36
Simmons, Dwayne D; Tong, Benton; Schrader, Angela D et al. (2010) Oncomodulin identifies different hair cell types in the mammalian inner ear. J Comp Neurol 518:3785-802
Fu, Benjamin; Le Prell, Colleen; Simmons, Dwayne et al. (2010) Age-related synaptic loss of the medial olivocochlear efferent innervation. Mol Neurodegener 5:53
Osman, Abdullah A; Schrader, Angela D; Hawkes, Aubrey J et al. (2008) Muscle-like nicotinic receptor accessory molecules in sensory hair cells of the inner ear. Mol Cell Neurosci 38:153-69
Gagnon, Patricia M; Simmons, Dwayne D; Bao, Jianxin et al. (2007) Temporal and genetic influences on protection against noise-induced hearing loss by hypoxic preconditioning in mice. Hear Res 226:79-91

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