Dopaminomimetic action of diphenylhydantoin in rat striatum: Effect on homovanillic acid and cyclic AMP levels

Lepore, Vito; Reda, N. Di; Defazio, Giovanni; Pedone, D; Giovine, A.; Lanzi, Cecilia Rodríguez; Tartaglione, Bruno; Livrea, Paolo

doi:10.1007/bf00431679

Cited by 5 publications

(2 citation statements)

References 17 publications

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“…Carbamazepine has a presynaptic dopaminereleasing action, both in vitro (Barros et al, 1986) and in vivo (Kaneko et al, 1993), which may well be a component of its anticonvulsant mechanism. Phenytoin leads to dopaminergic supersensitivity after long-term administration to rats (Lalonde, 1985; but see Lepore et al, 1985) and to dopamine-like orofacial dyskinesias in epileptic patients. Likewise, vigabatrin treatment of epilepsy has been sporadically linked to psychosis, with evidence of increased HVA levels in the CSF following acute (Ben-Menachem et al, 1989) but not chronic (Riekkinen et al, 1989) vigabatrin treatment and of increased *231-IBZM binding to Dz receptors in the basal ganglia of the left hemisphere of six chronic epileptics (Ring et al, 1992).…”

Section: Effects Of Chemoconvulsantsmentioning

confidence: 99%

The role of dopamine in epilepsy

Starr

1996

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The clinical benefits of dopamine agonists in the management of epilepsy can be traced back over a century, whilst the introduction of neuroleptics into psychiatry practice 40 years ago witnessed the emergence of fits as a side effect of dopamine receptor blockade. Epidemiologists noticed a reciprocal relationship between the supposed dopaminergic overactivity syndrome of schizophrenia and epilepsy, which came to be regarded as a dopamine underactivity condition. Early pharmacological studies of epilepsy employed nonselective drugs, that often did not permit dopamine's antiepileptic action to be clearly dissociated from that of other monoamines. Likewise, the biochemical search for genetic abnormalities in brain dopamine function, as predeterminants of spontaneous epilepsy, proved largely inconclusive. The discovery of multiple dopamine receptor families (D1 and D2), mediating opposing influences on neuronal excitability, heralded a new era of dopamine‐epilepsy research. The traditional anticonvulsant action of dopamine was attributed to D2 receptor stimulation in the forebrain, while the advent of selective D1 agonists with proconvulsant properties revealed for the first time that dopamine could also lower the seizure threshold from the midbrain. Whilst there is no immediate prospect of developing D2 agonists or D1 antagonists as clinically useful antiepileptics, there is a growing awareness that seizures might be precipitated as a consequence of treating other neurological disorders with D2 antagonists (schizophrenia) or D1 agonists (parkinsonism). © 1996 Wiley‐Liss, Inc.

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Section: Effects Of Chemoconvulsantsmentioning

confidence: 99%

The role of dopamine in epilepsy

Starr

1996

Synapse

234

155

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“…creasing, if any, effect on DA turnover. Although some authors (Lepore et al, 1985) reported a dopaminomimetic action of phenytoin and a subsensitivity of DA receptors after chronic administration of the drug, others (Lalonde, 1985) proposed a dopaminergic supersensitivity as a result of a long-term phenytoin administration.…”

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confidence: 99%

Homovanillic Acid and Prolactin in Plasma and CSF of Medicated Epileptic Patients

Kalfakis

Markianos²

1987

Epilepsia

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Homovanillic acid (HVA), the main dopamine metabolite, and prolactin (PRL) were estimated in plasma and cerebrospinal fluid (CSF) of 11 male epileptic patients treated with antiepileptic drugs and of 14 neurologic controls. A trend toward higher concentrations in plasma and lower concentrations in CSF in the patient group as compared with controls was observed for both parameters. The plasma to CSF ratios of HVA and PRL levels were significantly higher in the patient group. This shift may be due to an influence of the drugs on the blood-brain barrier (BBB) permeability. The PRL levels in the CSF correlated negatively to the HVA levels in CSF in the patient group only.

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