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J Neurophysiol (November 1, 2006). doi:10.1152/jn.00915.2006
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Submitted on August 28, 2006
Accepted on October 26, 2006

Development of spontaneous miniature EPSCs in mouse AVCN neurons over a critical period of afferent-dependent neuron survival

Yong Lu1, Julie A. Harris1, and Edwin W. Rubel2*

1 Virginia Merrill Bloedel Hearing Research Center, Department of Otolaryngology-HNS, Univ. of Washington, Seattle, Washington, United States
2 Univ. of Washington; Virginia Merrill Bloedel Hearing Research Center, Department of Otolaryngology-HNS, Univ. of Washington, Seattle, Washington, United States

* To whom correspondence should be addressed. E-mail: rubel{at}u.washington.edu.

During a critical period prior to hearing onset, cochlea ablation leads to massive neuronal death in the mouse anteroventral cochlear nucleus (AVCN), where cell survival is believed to depend on glutamatergic input. We investigated the development of spontaneous miniature excitatory postsynaptic currents (mEPSCs) in AVCN neurons using whole-cell patch clamp techniques during (P7) and after (P14, P21) this critical period. We also examined the effects of unilateral cochlea ablation on mEPSC development. The two main AVCN neuron types, bushy and stellate cells, were distinguished electrophysiologically. Bushy cell mEPSCs became more frequent and faster between P7 and P14/P21, but with little change in amplitude. Dendritic filtering of mEPSCs was not detected, as indicated by the lack of correlation between 10-90% rise times and decay time constants. Seven days after cochlea ablation at P7 or P14, mEPSCs in surviving bushy cells were similar to controls, except that rise and decay times were positively correlated (R=0.31 and 0.14 for surgery at P7 and P14, respectively). Consistent with this evidence for a shift of synaptic activity from the somata to the dendrites, SV2 staining (a synaptic vesicle marker) forms a ring around somata of control, but not experimental bushy cells. In contrast, mEPSCs of stellate cells showed few significant changes over these ages, with or without cochlea ablation. Taken together, mEPSCs in mouse AVCN bushy cells show dramatic developmental changes across this critical period, and cochlea ablation may lead to the emergence of excitatory synaptic inputs impinging on bushy cell dendrites.




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