methylatropine and Substance-Withdrawal-Syndrome

methylatropine has been researched along with Substance-Withdrawal-Syndrome* in 2 studies

Other Studies

2 other study(ies) available for methylatropine and Substance-Withdrawal-Syndrome

Article	Year
Muscarinic depression of synaptic transmission in the epileptogenic GABA withdrawal syndrome focus. Journal of neurophysiology, 2001, Volume: 85, Issue:5 The GABA withdrawal syndrome (GWS) is a model of local status epilepticus consecutive to the interruption of a prolonged GABA infusion into the rat somatomotor cortex. Bursting patterns in slices from GWS rats include intrinsic bursts of action potentials (APs) induced by intracellular depolarizing current injection and/or paroxysmal depolarization shifts (PDSs) induced by white matter stimulation. Possible changes in the effects of cholinergic drugs after in vivo induction of GWS were investigated on bursting cells (n = 30) intracellularly recorded in neocortical slices. In GWS slices, acetylcholine (Ach, 200-1000 microM) or carbachol (Cch, 50 microM) applications increased the number of bursts induced by depolarizing current injection while synaptically induced PDSs were significantly diminished (by 50-60%) or even blocked independently of the cholinergic-induced depolarization. The intrinsic burst facilitation and PDS depression provoked by Ach or Cch were mimicked by methyl-acetylcholine (mAch, 100-400 microM, n = 11), were reversed by atropine application (1-50 microM, n = 3), and were not mimicked by nicotine (50-100 microM, n = 4), indicating the involvement of muscarinic receptors. In contrast, in nonbursting cells from the same epileptic area (n = 42) or from equivalent area in control rats (n = 24), a nonsignificant muscarinic depression of EPSPs was induced by Cch and Ach. The mAch depression of excitatory postsynaptic potential (EPSPs) was significantly lower than that seen for PDSs in GWS rats. None of the cholinergic agonists caused bursting appearance in these cells. Therefore the present study demonstrates a unique implication of muscarinic receptors in exerting opposite effects on intrinsic membrane properties and on synaptic transmission in epileptiform GWS. Muscarinic receptor mechanisms may therefore have a protective role against the development and spread of epileptiform activity from the otherwise-activated epileptic focus. Topics: Action Potentials; Animals; Atropine Derivatives; Disease Models, Animal; Excitatory Postsynaptic Potentials; gamma-Aminobutyric Acid; Male; Motor Cortex; Muscarinic Agonists; Muscarinic Antagonists; Nicotine; Patch-Clamp Techniques; Pyramidal Cells; Rats; Rats, Wistar; Reaction Time; Receptors, Muscarinic; Status Epilepticus; Substance Withdrawal Syndrome; Synaptic Transmission	2001
Morphine abstinence syndrome: cholinergic mechanisms in the ventral periaqueductal gray of the dog. NIDA research monograph, 1984, Volume: 49 Topics: Acetylcholine; Animals; Atropine Derivatives; Carbachol; Dogs; Humans; Morphine; Morphine Dependence; Naloxone; Periaqueductal Gray; Receptors, Cholinergic; Substance Withdrawal Syndrome	1984

Article

Year

Muscarinic depression of synaptic transmission in the epileptogenic GABA withdrawal syndrome focus.

Journal of neurophysiology, 2001, Volume: 85, Issue:5

The GABA withdrawal syndrome (GWS) is a model of local status epilepticus consecutive to the interruption of a prolonged GABA infusion into the rat somatomotor cortex. Bursting patterns in slices from GWS rats include intrinsic bursts of action potentials (APs) induced by intracellular depolarizing current injection and/or paroxysmal depolarization shifts (PDSs) induced by white matter stimulation. Possible changes in the effects of cholinergic drugs after in vivo induction of GWS were investigated on bursting cells (n = 30) intracellularly recorded in neocortical slices. In GWS slices, acetylcholine (Ach, 200-1000 microM) or carbachol (Cch, 50 microM) applications increased the number of bursts induced by depolarizing current injection while synaptically induced PDSs were significantly diminished (by 50-60%) or even blocked independently of the cholinergic-induced depolarization. The intrinsic burst facilitation and PDS depression provoked by Ach or Cch were mimicked by methyl-acetylcholine (mAch, 100-400 microM, n = 11), were reversed by atropine application (1-50 microM, n = 3), and were not mimicked by nicotine (50-100 microM, n = 4), indicating the involvement of muscarinic receptors. In contrast, in nonbursting cells from the same epileptic area (n = 42) or from equivalent area in control rats (n = 24), a nonsignificant muscarinic depression of EPSPs was induced by Cch and Ach. The mAch depression of excitatory postsynaptic potential (EPSPs) was significantly lower than that seen for PDSs in GWS rats. None of the cholinergic agonists caused bursting appearance in these cells. Therefore the present study demonstrates a unique implication of muscarinic receptors in exerting opposite effects on intrinsic membrane properties and on synaptic transmission in epileptiform GWS. Muscarinic receptor mechanisms may therefore have a protective role against the development and spread of epileptiform activity from the otherwise-activated epileptic focus.

Topics: Action Potentials; Animals; Atropine Derivatives; Disease Models, Animal; Excitatory Postsynaptic Potentials; gamma-Aminobutyric Acid; Male; Motor Cortex; Muscarinic Agonists; Muscarinic Antagonists; Nicotine; Patch-Clamp Techniques; Pyramidal Cells; Rats; Rats, Wistar; Reaction Time; Receptors, Muscarinic; Status Epilepticus; Substance Withdrawal Syndrome; Synaptic Transmission

2001

Morphine abstinence syndrome: cholinergic mechanisms in the ventral periaqueductal gray of the dog.

NIDA research monograph, 1984, Volume: 49

Topics: Acetylcholine; Animals; Atropine Derivatives; Carbachol; Dogs; Humans; Morphine; Morphine Dependence; Naloxone; Periaqueductal Gray; Receptors, Cholinergic; Substance Withdrawal Syndrome

1984