ZIB

1

Digitale Medien

IVERSEN, L. ; FOSTER, A. C. ; HILL, R. G. ; [weitere]

Oxford, UK : Blackwell Publishing Ltd

Annals of the New York Academy of Sciences 648 (1992), S. 0

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ISSN: 1749-6632

Quelle: Blackwell Publishing Journal Backfiles 1879-2005

Thema: Allgemeine Naturwissenschaft

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1111/j.1749-6632.1992.tb24540.x

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2

Digitale Medien

Alterations in cerebral glutamic acid decarboxylase and3H-flunitrazepam binding during continuous treatment of rats for up to 1 year with haloperidol, sulpiride or clozapine (1987)

Rupniak, N. M. J. ; Prestwich, S. A. ; Horton, R. W. ; [weitere]

Springer

Journal of neural transmission 68 (1987), S. 113-125

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ISSN: 1435-1463

Schlagwort(e): Neuroleptics ; striatum ; substantia nigra ; GAD ; 3H-flunitrazepam binding

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Summary Rats were treated continuously for 12 months with therapeutically equivalent doses of haloperidol (1.4–1.6 mg/kg/day), sulpiride (102–109 mg/kg/day) or clozapine (24–27 mg/kg/day) and examined for alterations in brain glutamic acid decarboxylase (GAD) and3H-flunitrazepam binding. Administration of haloperidol, but not sulpiride or clozapine, for 6 or 12 months increased striatal GAD activity. None of the drug treatments altered nigral GAD activity when examined after 1, 3, 6, 9 or 12 months administration. The number of specific3H-flunitrazepam binding sites (Bmax) in striatal membrane preparations were not altered by 12 months administration of haloperidol, sulpiride or clozapine. Surprisingly, Bmax for3H-flunitrazepam binding to cerebellar membrane preparations was decreased-by 12 months administration of all drug treatments. The dissociation constant (Kd) for3H-flunitrazepam binding in striatal and cerebellar preparations was not altered. The ability of GABA (0.25–100 μM) alone, and in conjunction with sodium chloride (200 mM), to stimulate specific3H-flunitrazepam binding in striatal and cerebellar preparations was unaltered by haloperidol, sulpiride or clozapine administration for 12 months. The selective effect of haloperidol, but not sulpiride or clozapine, treatment on striatal GAD activity parallels the ability of haloperidol, but not sulpiride or clozapine, to induce striatal dopamine receptor supersensitivity in the same animals. The actions of haloperidol may reflect its greater ability to induce tardive dyskinesia compared to sulpiride or clozapine.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF01244643

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3

Digitale Medien

Cholinergic manipulation of perioral behaviour induced by chronic neuroleptic administration to rats (1983)

Rupniak, N. M. J. ; Jenner, P. ; Marsden, C. D.

Springer

Psychopharmacology 79 (1983), S. 226-230

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ISSN: 1432-2072

Schlagwort(e): Neuroleptics ; Perioral responses ; Cholinergic agents ; Tardive dyskinesia ; Acute dystonic reactions ; Rat

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Rats treated continuously for 4 months with haloperidol (1.4–1.6 mg/kg/day), trifluoperazine (4.5–5.1 mg/kg/day), or sulpiride (102–110 mg/kg/day), but not clozapine (23–26 mg/kg/day), exhibited an increased frequency of chewing jaw movements. Chewing in both control and haloperidol-treated rats was increased by acute administration of the cholinergic agents pilocarpine or physostigmine. Physostigmine or pilocarpine also induced abnormal gaping jaw movements; physostigmine-induced gaping was more prevalent in haloperidol-treated rats than control rats receiving physostigmine alone. Acute administration of the anticholinergic agents scopolamine and atropine decreased chewing in control animals and reduced haloperidol-induced chewing to control values or below. The effects of these cholinergic manipulations suggest that neuroleptic-induced perioral responses in rats do not resemble tardive dyskinesia in man.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00427817

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4

Digitale Medien

Differential effects of continuous administration for 1 year of haloperidol or sulpiride on striatal dopamine function in the rat (1984)

Rupniak, N. M. J. ; Mann, S. ; Hall, M. D. ; [weitere]

Springer

Psychopharmacology 84 (1984), S. 503-511

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ISSN: 1432-2072

Schlagwort(e): Haloperidol ; Sulpiride ; Striatum ; Supersensitivity ; Dopamine receptors ; Rat

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Administration of haloperidol (1.4–1.6 mg/kg/day) for up to 12 months or sulpiride (102–109 mg/kg/day) for between 6 and 12 months increased the frequency of purposeless chewing jaw movements in rats. N,n-propylnorapomorphine (NPA) (0.25–2.0 mg/kg SC) did not induce hypoactivity in haloperidol-treated rats at any time; sulpiride treatment for 9 and 12 months caused a reduction in the ability of NPA to induce hypoactivity. Haloperidol, but not sulpiride, treatment enduringly inhibited low dose apomorphine effects (0.125 mg/kg SC). After 12 months, sterotypy induced by high doses of apomorphine (0.5–1.0 mg/kg) was exaggerated in haloperidol-, but not sulpiride-treated rats. Bmax for specific striatal 3H-spiperone binding was increased by haloperidol, but not sulpiride, treatment throughout the study. Bmax for 3H-NPA binding was elevated only after 12 months of both haloperidol and sulpiride treatment. Bmax for 3H-piflutixol binding was not alfered by chronic haloperidol or sulpiride treatment. Striatal dopamine-stimulated adenylate cyclase activity was inhibited for the 1st month of haloperidol treatment, thereafter returning to control levels; dopamine stimulation was increased after 12 months of sulpiride treatment. Striatal acetylcholine content was increased after 3 and 12 months of treatment with haloperidol, but was not affected by sulpiride. Chronic administration of sulpiride does not induce identical changes in striatal dopamine function to those caused by haloperidol.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00431457

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5

Digitale Medien

Differential alterations in striatal dopamine receptor sensitivity induced by repeated administration of clinically equivalent doses of haloperidol, sulpiride or clozapine in rats (1984)

Rupniak, N. M. J. ; Kilpatrick, G. ; Hall, M. D. ; [weitere]

Springer

Psychopharmacology 84 (1984), S. 512-519

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ISSN: 1432-2072

Schlagwort(e): Clozapine ; Sulpiride ; Haloperidol ; Dopamine receptors ; Sterotypy

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Rats received therapeutically equivalent doses of either haloperidol (1.7–1.9 mg/kg/day), sulpiride (112–116 mg/kg/day) or clozapine (30–35 mg/kg/day) continuously for 4 weeks. Treatment with haloperidol, but not sulpiride or clozapine, caused inhibition of stereotyped behaviour induced by apomorphine (0.125–0.25 mg/kg SC). Following drug withdrawal for up to 7 days, haloperidol and sulpiride, but not clozapine treatment caused an exaggeration of stereotyped behaviour induced by apomorphine. Bmax values for striatal 3H-spiperione binding were erevated in animals treated for 2 and 4 weeks with haloperidol, but not with sulpiride or clozapine. Following drug withdrawal, haloperidol, but not sulpiride or clozapine, treatment caused an increase in Bmax for striatal 3H-piperone binding. Bmax values for striatal 3H-NPA binding revealed no change during haloperidol or clozapine treatment. Sulpiride treatment for 1 week caused an increase in Bmax for 3H-NPA binding, which returned to control levels at 2 and 4 weeks. Following drug withdrawal, there was an increase in Bmax for 3H-NPA binding in rats treated with haloperidol and sulpiride, but not clozapine. On continuous treatment and following withdrawal from haloperidol, sulpiride, or clozapine the ability of dopamine to stimulate striatal adenylate cyclase activity did not differ from that in control animals. Repeated administration of sulpiride or clozapine may not induce striatal dopamine receptor supersensitivity when given in clinically relevant doses, although haloperidol does.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00431458

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6

Digitale Medien

Pharmacological characterisation of spontaneous or drug-associated purposeless chewing movements in rats (1985)

Rupniak, N. M. J. ; Jenner, P. ; Marsden, C. D.

Springer

Psychopharmacology 85 (1985), S. 71-79

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ISSN: 1432-2072

Schlagwort(e): Dopamine ; Acetylcholine ; Acute dystonia ; Peri-oral behaviour ; Rat

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Continuous administration of haloperidol, sulpiride, or cis-flupenthixol, but not of domperidone or apomorphine, to Wistar rats for up to 3 weeks caused an increase in spontaneous purposeless chewing movements. Treatment with physostigmine and pilocarpine, but not neostigmine, for up to 3 weeks increased chewing, whilst scopolamine decreased chewing. Metergoline and cyproheptadine, but not quipazine, increased chewing after only 1 and 7 days but not thereafter. Chewing was not altered following treatment with compounds acting on GABA or noradrenaline systems or by a range of non-neuroleptic agents inducing dystonia in man. The enhancement of chewing induced by neuroleptic and cholinomimetic drugs was reduced by acute treatment with scopolamine, and reverted to control levels following drug withdrawal. Neuroleptic-induced purposeless chewing in Wistar rats appears to be primarily influenced by cerebral dopamine and acetylcholine function and may resemble acute dystonia, rather than tardive dyskinesia.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00427326

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7

Digitale Medien

Comparison of the effects of four cholinomimetic agents on cognition in primates following disruption by scopolamine or by lists of objects (1989)

Rupniak, N. M. J. ; Steventon, M. J. ; Field, M. J. ; [weitere]

Springer

Psychopharmacology 99 (1989), S. 189-195

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ISSN: 1432-2072

Schlagwort(e): Delayed nonmatching-to-sample ; Spatial delayed response ; Cholinomimetics ; Scopolamine ; Rhesus monkey

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract The ability of four central cholinomimetics to reverse a scopolamine-induced spatial memory impairment or to improve visual recognition memory in primates was examined. Physostigmine (0.04–0.08 mg/kg IM) fully reversed the effects of scopolamine (0.03 mg/kg). Coadministration of pilocarpine (3.0–5.0 mg/kg) caused partial reversal of the scopolamine impairment after intermediate or long retention intervals (10 or 20 s). Treatment with arecoline (0.1–1.8 mg/kg) or nicotine (1.0–2.0 mg/kg) generally did not reverse the effects of scopolamine. A task in which memory could be taxed by increasing the number of visual stimuli presented appeared more sensitive to the effects of cholinomimetics on cognition than the scopolamine reversal model. In this paradigm treatment with physostigmine (0.001, 0.01 or 0.03 mg/kg) increased choice accuracy from about 55 to 70% correct. Arecoline improved performance at one dose only (0.1 mg/kg) which also induced marked adverse side-effects (salivation and tremor). Pilocarpine improved performance in the dose range 0.125–0.35 mg/kg, but not at higher doses which also induced marked salivation. Treatment with nicotine (0.001–2.0 mg/kg tended to improve performance but this did not reach statistical significance. The relevance of these findings for studies in man and for animal models of dementia is discussed.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00442806

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8

Digitale Medien

Enhanced performance of spatial and visual recognition memory tasks by the selective acetylcholinesterase inhibitor E2020 in rhesus monkeys (1997)

Rupniak, N. M. J. ; Tye, Spencer J. ; Field, Mark J.

Springer

Psychopharmacology 131 (1997), S. 406-410

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ISSN: 1432-2072

Schlagwort(e): Key words Tacrine ; Alzheimer’s disease ; Palliative therapy ; Cognition ; Acetylcholine

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Hepatotoxicity limits the clinical utility of the cholinesterase inhibitor tacrine as a palliative therapy for Alzheimer’s disease. The present studies examined the effects of E2020, a selective acetylcholinesterase inhibitor not associated with liver toxicity in man, on cognitive performance in rhesus monkeys using tasks employed previously to evaluate tacrine and other cholinomimetic agents. The ability of E2020 to prevent the induction of a cognitive impairment by the muscarinic receptor antagonist scopolamine was assessed using an automated spatial delayed response task. Coadministration of E2020 (0.5–1.75 mg/kg) caused a dose-dependent reversal of the scopolamine (0.03 mg/kg) induced impairment observed after retention intervals of 10 and 20 s. At the highest dose of E2020 examined (1.75 mg/kg), choice accuracy approached normal control levels. In this dose range, E2020 was well tolerated, but at the higher dose of 2 mg/kg, cholinergic side-effects were apparent. The effect of E2020 on choice accuracy in a visual recognition task was also assessed as this task does not require the use of scopolamine to disrupt performance and beneficial effects of cholinomimetics can therefore be detected at lower doses than in the spatial memory paradigm. In this task, administration of E2020 increased choice accuracy from 59 ± 1% correct to up to 71 ± 2% at doses of 0.03 and 0.05 mg/kg. No observable adverse effects were induced by E2020 in this dose range. The ability of E2020 to improve performance in these cognitive tasks resembles the profile of other cholinesterase inhibitors, including tacrine, that also improve cognitive function in Alzheimer’s disease patients. Because of its more favourable clinical safety profile, E2020 may provide a significantly improved palliative therapy for dementia.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/s002130050310

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9

Digitale Medien

Drug-induced purposeless chewing: animal model of dyskinesia or nausea? (1990)

Rupniak, N. M. J. ; Tye, S. J. ; Iversen, S. D.

Springer

Psychopharmacology 102 (1990), S. 325-328

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ISSN: 1432-2072

Schlagwort(e): Dyskinesia ; Nausea ; Squirrel monkey ; Emesis

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract Drug-induced purposeless chewing movements in rodents are often considered to represent movement disorders or dyskinesias. We have compared the ability of drugs to induce chewing and retching or emesis in squirrel monkeys; such studies are not possible in rodents, which do not vomit. Acute administration of oxotremorine (3.3–33 µg/kg IM), SKF38393 (1–30 mg/kg SC) or ipecacuanha (0.5–0.75 mg/kg PO) caused dose-related increases in purposeless chewing which was frequently associated with retching and emesis. Treatment with haloperidol (0.015–0.06 mg/kg IM) did not induce chewing. Rather, haloperidoldecreased spontaneous chewing at doses of 0.03 and 0.06 mg/kg. Our findings indicate that at least some drug-induced oral behaviours in rodents may reflect nausea rather than dyskinesia.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF02244098

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10

Digitale Medien

Acute dystonia induced by neuroleptic drugs (1986)

Rupniak, N. M. J. ; Jenner, P. ; Marsden, C. D.

Springer

Psychopharmacology 88 (1986), S. 403-419

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ISSN: 1432-2072

Schlagwort(e): Dystonia ; Neuroleptics ; Dyskinesia ; Animal models

Quelle: Springer Online Journal Archives 1860-2000

Thema: Medizin

Notizen: Abstract About 2.5% of patients treated with neuroleptic drugs develop acute dystonia within 48 h of commencing therapy. The symptoms remit on drug withdrawal or following anticholinergic therapy. Acute dystonia can also be reliably induced in many primate species by neuroleptic treatment with comparable time course, symptomatology and pharmacological characteristics to those observed in man. In general, New World monkeys appear more susceptible to acute dystonia than Old World primates. It is at present not clear whether all primates, including man, would exhibit dystonia if a sufficiently high dose of neuroleptic was administered. Alternatively, some unknown, possibly species-specific or even genetic, factors may determine an individual's susceptibility to develop dystonia. Use of a rodent model of dystonia might enable more detailed analysis of biochemical correlates of dystonic behaviour. Whilst rodents do not exhibit overt dystonic behaviour after neuroleptic treatment, they may develop oral dyskinesias which bear a close pharmacological similarity to dystonia in man and primates. However, it is not known whether chewing induced by neuroleptic drugs in rats resembles acute dystonia in primates or whether this is another movement disorder possibly unique to rodent species. The pathophysiology of acute dystonia remains unknown, but may involve striatal dopaminergic and cholinergic function. In view of the close similarity between dystonia in man and other primates, studies on the mechanisms whereby neuroleptic drugs cause acute dystonic reactions in monkeys may give some clues to the pathogenesis of spontaneous dystonia in man.

Materialart: Digitale Medien

URL: http://dx.doi.org/10.1007/BF00178501

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