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J Neurophysiol 99: 1712-1722, 2008. First published February 13, 2008; doi:10.1152/jn.00038.2008
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Organization and Properties of GABAergic Neurons in Solitary Tract Nucleus (NTS)

Timothy W. Bailey, Suzanne M. Appleyard, Young-Ho Jin and Michael C. Andresen

Department of Physiology and Pharmacology, Oregon Health and Science University, Portland, Oregon

Submitted 10 January 2008; accepted in final form 12 February 2008

Cranial visceral afferents enter the brain at the solitary tract nucleus (NTS). GABAergic neurons are scattered throughout the NTS, but their relation to solitary tract (ST) afferent pathways is imprecisely known. We hypothesized that most GABAergic NTS neurons would be connected only indirectly to the ST. We identified GABAergic neurons in brain stem horizontal slices using transgenic mice in which enhanced green fluorescent protein (EGFP) expression was linked to glutamic acid decarboxylase expression (GAD+). Finely graded electrical shocks to ST recruit ST-synchronized synaptic events with all-or-none thresholds and individual waveforms did not change with greater suprathreshold intensities—evidence consistent with initiation by single afferent axons. Most (~70%) GAD+ neurons received ST-evoked excitatory postsynaptic currents (EPSCs) that had minimally variant latencies (jitter, SD of latency <200 µs) and waveforms consistent with single, direct ST connections (i.e., monosynaptic). Increasing stimulus intensity evoked additional ST-synchronized synaptic responses with jitters >200 µs including inhibitory postsynaptic currents (IPSCs), indicating indirect connections (polysynaptic). Shocks of suprathreshold intensity delivered adjacent (50–300 µm) to the ST failed to excite non-ST inputs to second-order neurons, suggesting a paucity of axons passing near to ST that connected to these neurons. Despite expectations, we found similar ST synaptic patterns in GAD+ and unlabeled neurons. Generally, ST information that arrived indirectly had small amplitudes (EPSCs and IPSCs) and frequency-dependent failures that reached >50% for IPSCs to bursts of stimuli. This ST afferent pathway organization is strongly use-dependent—a property that may tune signal propagation within and beyond NTS.


Address for reprint requests and other correspondence: M. C. Andresen, Dept. of Physiology and Pharmacology, Oregon Health and Science Univ., Portland, OR 97239-3098 (E-mail: andresen.ohsu{at}gmail.com)




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