Abstract

Cellular mechanisms underlying neurotoxic actions of methylmercury (MeHg) in the peripheral and central nervous system will be studied in mammals using intracellular microelectrode recording techniques and radiochemical flux determinations. The objectives are to determine: a) whether MeHg produces changes in synaptic transmission in cortical neurons which correspond to those observed in peripheral, somatic nerves; b) whether MeHg blocks nerve Ca2+ channels, and if so whether the ionic selectivity of the channel is altered, whether the effects are preferential for a particular type of Ca2+ channel, and whether congeners of MeHg produce similar effects; or whether MeHg blocks Ca2+ uptake or induces Ca2+ release from neuronal mitochondria and/or smooth endoplasmic reticulum; d) whether MeHg enters the nerve terminal, if so, by what path it enters, and where it goes; e) whether MeHg produces postsynaptic effects at the neuromuscular junction; f) to what extent do the electrophysiological changes described for MeHg occur when a permanently uncharged organic, or a monovalent inorganic form of Hg is used; and g) whether electrophysiological changes described with acute application of MeHg occur when animals are treated chronically with MeHg? Intracellular microelectrode recordings including voltage clamp and quantitative iontophoresis will be made from the somatic neuromuscular junction of the rat and from mossy fiber/CA3 pyramidal cell excitatory synapses in isolated hippocampal slices of the guinea pig. Effects of MeHg on nerve-evoked and spontaneous release will be measured. Effects of MeHg on Ca2+- driven action potentials in hippocampal cells will be studied. Effects of MeHg on Ca2+ currents in N1E-115 neuroblastoma cells using whole cell patch voltage clamp will be used to determine if MeHg blocks Ca2+ channels. Effects of MeHg on Ca2+ channel ion selectivity will be assessed using uptake of radiolabelled Ca, Sr and Ba. Comparative effects of structurally-related mercurials on calcium influx will also be studied. Synaptosomes will also be used to test whether MeHg enters the nerve terminal, and if so how MeHg interacts with intracellular Ca2+ regulatory systems in the nerve terminal. Measurements of nerve-evoked and spontaneous release from motor nerves of rats treated chronically with MeHg will be used to assess the relevance to chronic MeHg neurotoxicity of the changes described previously for acute intoxication. Results from the proposed studies should provide answers to questions concerning the interaction of MeHg with cortical synaptic transmission, the interaction, with Ca2+ in synaptic transmission at both membrane and intracellular loci, and the effects of chronic MeHg poisoning on synaptic transmission.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Modified Research Career Development Award (K04)
Project #
1K04ES000178-01
Application #
3072743
Study Section
Toxicology Study Section (TOX)
Project Start
1987-12-01
Project End
1992-11-30
Budget Start
1987-12-01
Budget End
1988-11-30
Support Year
1
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Michigan State University
Department
Type
Schools of Veterinary Medicine
DUNS #
193247145
City
East Lansing
State
MI
Country
United States
Zip Code
48824

  Publications

Spitsbergen, J M; Atchison, W D (1995) The paralytic agent 2,4-dithiobiuret decreases open time of murine skeletal muscle acetylcholine receptor channels. J Pharmacol Exp Ther 272:645-51
Yuan, Y; Atchison, W D (1993) Disruption by methylmercury of membrane excitability and synaptic transmission of CA1 neurons in hippocampal slices of the rat. Toxicol Appl Pharmacol 120:203-15
Shafer, T J; Atchison, W D (1992) Effects of methylmercury on perineurial Na+ and Ca(2+)-dependent potentials at neuromuscular junctions of the mouse. Brain Res 595:215-9
Hare, M F; Atchison, W D (1992) Differentiation between alterations in plasma and mitochondrial membrane potentials in synaptosomes using a carbocyanine dye. J Neurochem 58:1321-9
Hewett, S J; Atchison, W D (1992) Effects of charge and lipophilicity on mercurial-induced reduction of 45Ca2+ uptake in isolated nerve terminals of the rat. Toxicol Appl Pharmacol 113:267-73
Atchison, W D; Geary, T G; Manning, B et al. (1992) Comparative neuromuscular blocking actions of levamisole and pyrantel-type anthelmintics on rat and gastrointestinal nematode somatic muscle. Toxicol Appl Pharmacol 112:133-43
Williams, K D; Peterson, R E; Atchison, W D (1992) High dose refractoriness to the neuromuscular toxicity of dithiobiuret in rats. Neurotoxicology 13:331-45
Hewett, S J; Atchison, W D (1992) Specificity of Lambert-Eaton myasthenic syndrome immunoglobulin for nerve terminal calcium channels. Brain Res 599:324-32
Hewett, S J; Atchison, W D (1992) Disruption of synaptosomal calcium channel function by Lambert-Eaton myasthenic immunoglobulin is serum-dependent. Brain Res 599:317-23
Hewett, S J; Atchison, W D (1991) Serum and plasma from patients with Lambert-Eaton Myasthenic Syndrome reduce depolarization-dependent uptake of 45Ca2+ into rat cortical synaptosomes. Brain Res 566:320-4

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