Abstract

The long-term goal of this project is to elucidate the integrative function of muscarinic and peptidergic synapses in bullfrog sympathetic ganglia. The bullfrog was chosen for study because its anatomical features are optimal for electrophysiological experiments that can be performed at the cellular level and directly related to the control of vascular tone and glandular secretion. The proposed experiments exploit the fact that paravertebral sympathetic neurons in the bullfrog are organized into 2 major subsystems, B and C, that can be identified by their axonal conduction velocities, and selectively activated due to the anatomical separation of their preganglionic inputs. These cell types are further distinguished by their expression of muscarinic synapses and neuropeptides, and by their functional roles. The experiments will employ electrophysiological methods to study isolated preparations containing either ganglia and their end-organs, ganglia alone, or end-organs alone, and to study dissociated neurons in primary cell culture. The proposal has 3 specific aims: 1) To test the hypothesis that co-transmitters endow the vasomotor C system with variable synaptic gain that is regulated by temporal patterns of preganglionic activity. The hypothetical model postulates that synapses in the ganglia and at end-organs function as 2 variable gain stages in series. In ganglia, acetylcholine (ACH) and luteinizing hormone releasing hormone (LHRH) are co-released to produce a nicotinic epsp, a slow muscarinic ipsp, and a slow peptidergic epsp. Temporal interactions between the 2 slow synaptic potentials are hypothesized to control ganglionic gain. In the periphery, it is postulated that the release of the co-transmitters epinephrine (EPI) and neuropeptide Y (NPY) is differentially regulated by activity. When NPY is released, it enhances end-organ gain by potentiating vascular responses to EPI. 2) To test the hypotheses that the B system innervates cutaneous mucous glands and that calcitonin gene-related peptide (CGRP) is both a ganglionic co-transmitter that mediates a slow epsp and a trophic factor that regulates the expression of nicotinic ACH receptors. 3) To test the hypothesis that LHRH released by preganglionic C fibers acts heterosynaptically to increase the gain of synapses between pre- and postganglionic B neurons. Results of the proposed studies will provide a conceptual framework for understanding the integrative function of synaptic co-transmission in more complex circuits including mammalian autonomic ganglia and the brain.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS021065-07A2
Application #
3401842
Study Section
Neurological Sciences Subcommittee 1 (NLS)
Project Start
1984-07-01
Project End
1995-09-29
Budget Start
1991-09-30
Budget End
1992-09-29
Support Year
7
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
University of Pittsburgh
Department
Type
Schools of Medicine
DUNS #
053785812
City
Pittsburgh
State
PA
Country
United States
Zip Code
15213

  Publications

Springer, Mitchell G; Kullmann, Paul H M; Horn, John P (2015) Virtual leak channels modulate firing dynamics and synaptic integration in rat sympathetic neurons: implications for ganglionic transmission in vivo. J Physiol 593:803-23
Rimmer, Katrina; Horn, John P (2010) Weak and straddling secondary nicotinic synapses can drive firing in rat sympathetic neurons and thereby contribute to ganglionic amplification. Front Neurol 1:130
Kullmann, Paul H M; Horn, John P (2010) Homeostatic regulation of M-current modulates synaptic integration in secretomotor, but not vasomotor, sympathetic neurons in the bullfrog. J Physiol 588:923-38
Kullmann, Paul H M; Horn, John P (2010) Vasomotor sympathetic neurons are more excitable than secretomotor sympathetic neurons in bullfrog paravertebral ganglia. Auton Neurosci 155:19-24
Li, Chen; Horn, John P (2008) Differential Inhibition of Ca2+ channels by alpha2-adrenoceptors in three functional subclasses of rat sympathetic neurons. J Neurophysiol 100:3055-63
Horn, J P; Kullmann, P H M (2007) Dynamic Clamp Analysis of Synaptic Integration in Sympathetic Ganglia. Neirofiziologiia 39:423-429
Headley, Drew B; Suhan, Nadine M; Horn, John P (2007) Different subcellular distributions of the vesicular monoamine transporter, VMAT2, in subclasses of sympathetic neurons. Brain Res 1129:156-60
Li, Chen; Horn, John P (2006) Physiological classification of sympathetic neurons in the rat superior cervical ganglion. J Neurophysiol 95:187-95
Kullmann, Paul H M; Horn, John P (2006) Excitatory muscarinic modulation strengthens virtual nicotinic synapses on sympathetic neurons and thereby enhances synaptic gain. J Neurophysiol 96:3104-13
Headley, Drew B; Suhan, Nadine M; Horn, John P (2005) Rostro-caudal variations in neuronal size reflect the topography of cellular phenotypes in the rat superior cervical sympathetic ganglion. Brain Res 1057:98-104

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