Pharmacological Studies on Lamotrigine, A Novel Potential Antiepileptic Drug

Summary: More than 50 million persons worldwide suffer from epilepsy, many of whom are refractory to treatment with standard antiepileptic drugs (AEDs Although epilepsy affects more than 50 million persons worldwide (l), the development of new pharmacologic interventions has lagged behind that of many other therapeutic categories. Until recently, physicians have had available a relatively limited armamentarium of antiepileptic drugs (AEDs) to treat patients with seizure disorders. This group of "standard" AEDs includes phenytoin (PHT), carbamazepine (CBZ), valproate (VPA), barbiturates such as phenobarbital (PB) and primidone (PRM), certain benzodiazepines (BZDs), and ethosuximide (ESM). Most of these agents have a limited spectrum of antiepileptic activity, and all have certain negative properties that limit their utility and complicate patient management. At least 25% of epilepsy patients remain refractory to these AEDs ( 2 ) . Seirecently been discovered. FBM appears to be active at the strychnine-insensitive glycine binding site of the NMDA receptor. TPM is active on the kainate/AMPA subtype of glutamate receptor and at a potentially novel site on the GABAA receptor. For several reasons, availability of a single AED with multiple mechanisms of action may be preferred over availability of multiple AEDs with single mechanisms of action. These reasons include ease of titration, lack of drugdrug interactions, and reduced potential for pharmacodynamic tolerance. Key Words: Anticonvulsants-Drug screening -Neurotransmitters -Phenytoin -Ethosuximide-Topiramate-Valproate-Benzodiazepines-Barbitu-zure control in many more patients is achieved only at the expense of various types and severities of AEDrelated adverse effects. The need for new AEDs with improved clinical profiles is therefore quite clear.Fortunately, the present decade has been marked by a number of advances in AED development. Since 1990, several novel AEDs have been commercialized in one or more countries and are in the process of evaluation for worldwide registrations. These include vigabatrin (VGB), lamotrigine (LTG), gabapentin (GBP), tiagabine (TGB), felbamate (FBM), and topiramate (TPM). This report briefly discusses the preclinical models supporting the clinical evaluation of these AEDs, reviews the presently proposed mechanisms of old and new AEDs, somewhat more closely examines the recently emerging mechanistic profile of the clinically promising new AED TPM, and offers some observations about the significance of mechanism findings from the scientific and the clinical perspective.

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“…LTG is active against tonic extension seizures in the MES test but is ineffective against scPTZ-induced clonus (40).…”

Section: Ltgmentioning

confidence: 99%

Clinical Significance of Animal Seizure Models and Mechanism of Action Studies of Potential Antiepileptic Drugs

1997

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“…It is available in several European countries and is awaiting FDA approval in the United States. Its preclinicd profile appears to be most similar to phenytoin (84). There have been several published safety and efficacy studies on lamotrigine in patients with epilepsy.…”

Section: Lamotriginementioning

confidence: 99%

“…In controlled clinical hids lamotrigine has demonstrated eflicacy in refractory patients with various seizures types (86) and refractory partial epilepsies (85,87). Chronic toxicity studies in rats and primates at doses of up to 20-125 mg/(kg day) have showed no toxic effects (84). The most frequently reported side-effects were diplopia, drowsiness, ataxia and headache (87).…”

Section: Lamotriginementioning

confidence: 99%

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Advances in pharmacotherapy: recent developments in the treatment of epilepsy

Graves

Leppik

1993

J Clin Pharm Ther

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SUMMARY Epilepsy is a disorder of the central nervous system in which the clinical symptoms are recurrent seizures. An increased understanding of the underlying mechanism of seizures and more definitive diagnostic procedures have improved the care of the patient with epilepsy. An improved classification of various seizure types, including specific epilepsy syndromes has helped optimize use of the standard antiepileptic drugs. Research on the mechanism of seizures has led to new antiepileptic drugs. More definitive diagnostic procedures have led to more accurate identification of patients likely to benefit from epilepsy surgery. This review focuses on these areas.

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“…It is generally considered at present that the clinical success of a new antiarrhythmic agent would require a significant redress of the limitations of presently available therapy. During the course ofpharmacological studies at the Wellcome Research Laboratories, it was observed that certain phenyl diamino-1,2,4 triazines possessed anticonvulsant activity, a property attributable to the ability of these agents to modulate neuronal sodium transport (Miller et al, 1984;Leach et al, 1985). Preliminary evaluation demonstrated that some of these chemically novel triazines were also able to reduce, in a concentration-dependent fashion, the sodium-dependent rate of rise ofphase 0 of the cardiac action potential, an action ascribed as a class 1 antiarrhythmic action (Vaughan Williams, 1981).…”

Section: Introductionmentioning

confidence: 99%

BW A256C, a chemically novel class 1 antiarrhythmic agent. A comparison of in vitro and in vivo activity with other class 1 antiarrhythmic agents

Allan¹,

Donoghue

Follenfant

et al. 1986

British J Pharmacology

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1 BW A256C (5(3)-amino-6-(2,3-dichlorophenyl)-2,3(2,5)-dihydro-3(5)-imino-2-isopropyl-1,2,4-triazine) is a novel class 1 antiarrhythmic agent designed to combine the features ofpotency with reduced central nervous system penetration. 2 BW A256C reduced the maximum rate of depolarization of guinea-pig ventricle and dog Purkinje fibres in vitro (EC5o, 2.2 x 10-6 M and 1.8 x 10-6 M, respectively), being significantly more potent than quinidine, lidocaine, disopyramide and flecainide. BW A256C was also more potent than these agents at inhibiting aconitine-induced arrhythmias in anaesthetized rats; however, unlike these agents, BW A256C was devoid of hypotensive activity at antiarrhythmic doses. 3 In anaesthetized dogs, intravenous administration of BW A256C (0.25-1 mg kg-') caused a dosedependent suppression of ventricular arrhythmias that occurred on reperfusion of an occluded coronary artery. 4In conscious dogs, intravenous infusion (total dose, 1.5 mg kg 1) or oral administration of BW A256C (1.25-5mg kg-') caused dose-dependent suppression of the ventricular ectopic activity that occurred following 20-24 h of permanent coronary artery ligation. 5In the conscious dog, BWA256C was approximately 7 times more potent and was also longer acting than flecainide. 6 Administration of BW A256C was not associated with any evidence of peripheral or CNS toxicity. However, plasma levels 3-4 times greater than the antiarrhythmic levels were associated with a proarrhythmic activity.

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Pharmacological Studies on Lamotrigine, A Novel Potential Antiepileptic Drug

Cited by 182 publications

References 6 publications

Clinical Significance of Animal Seizure Models and Mechanism of Action Studies of Potential Antiepileptic Drugs

Clinical Significance of Animal Seizure Models and Mechanism of Action Studies of Potential Antiepileptic Drugs

Advances in pharmacotherapy: recent developments in the treatment of epilepsy

BW A256C, a chemically novel class 1 antiarrhythmic agent. A comparison of in vitro and in vivo activity with other class 1 antiarrhythmic agents

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