Remacemide Hydrochloride : A Double-Blind, Placebo-Controlled, Safety and Tolerability Study in Patients With Acute Ischemic Stroke

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Stroke. 1999;30:1796-1801

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(Stroke. 1999;30:1796-1801.)
© 1999 American Heart Association, Inc.

Original Contributions

Remacemide Hydrochloride

A Double-Blind, Placebo-Controlled, Safety and Tolerability Study in Patients With Acute Ischemic Stroke

A. G. Dyker, MD, MRCP K. R. Lees, MD, FRCP

From the Acute Stroke Unit, University Department of Medicine and Therapeutics, Gardiner Institute, Western Infirmary, Glasgow, G11 6NT Scotland, UK.

Correspondence to Dr A.G. Dyker, Acute Stroke Unit, University Department of Medicine and Therapeutics, Gardiner Institute, Western Infirmary, Glasgow, G11 6NT Scotland, UK. E-mail AD47Q{at}clinmed.gla.ac.uk

Background and Purpose—Remacemide hydrochloride and itsprincipal active desglycinyl metabolite are low-affinity noncompetitive N-methyl-D-aspartate(NMDA)-receptor channel blockers. Remacemide hydrochloride hasdemonstrated neuroprotection in animal models of hypoxia andischemic stroke. This study assessed the safety, tolerability,and pharmacokinetics of ascending doses of remacemide hydrochloridein patients with recent onset (within 12 hours) ischemic stroke.

Methods—This was a placebo-controlled, dose escalating,parallel group study. Groups of 8 patients (6 active, 2 placebo)were planned to receive twice-daily treatment, with l00 mg,200 mg, 300 mg, 400 mg, 500 mg, or 600 mg remacemide hydrochloridegiven as 2 intravenous infusions followed by 6 days' oral treatment. Patientswho were unable to swallow discontinued study medication but continuedto be monitored for safety; these patients were replaced. A CTor MRI scan was performed within 48 hours of admission to establish thecause of focal neurological deficit. Patients with ischemic strokecontinued in the study. Patients with other causes of focal neurologicaldeficit were withdrawn and replaced. Because the frequency ofdysphagia after stroke in the first dose group (l00 mg BID)was higher than had been anticipated, the protocol was amendedso that subsequent dose groups received 6 intravenous infusions(2 doses per day for 3 days). Neurological and functional outcomedata were collected, but the study was not powered to demonstratedrug efficacy. Patient safety was assessed by clinical observation, laboratorytests, and ECGs, while tolerability was assessed by recordingadverse events. Blood sampling was included to determine plasmaconcentrations of remacemide and the desglycinyl metaboliteat fixed points during the dosing period.

Results—The most common adverse events considered by the investigatorto be possibly treatment related were related to the centralnervous system (CNS), and these events appeared to increase withdose. Four patients were withdrawn from the study because of CNS-relatedevents: 1 in the placebo group, 1 in the 500 mg BID group, and2 in the 600 mg BID group. Infusion site reactions and gastrointestinalupset were also reported and considered to be treatment related.One patient in the placebo group and 4 patients in the 600 mgBID dose group experienced vomiting, whereas this event was notreported by patients in the other dose groups.

Conclusions—On the evidence of this study, the maximum well-tolerateddose for remacemide hydrochloride in acute stroke is 400 mgBID. Doses of 200 mg BID or higher attained the putative neuroprotectiveplasma concentrations of remacemide predicted from animal models(250 to 600 ng/mL). The expected gradual accumulation of activemetabolite might suggest that optimal neuroprotective concentrationsare unlikely to be achieved within the early hours of treatmentat this dose. However, plasma concentrations do not directly reflectbrain concentrations, because studies in rats show that remacemideand the desglycinyl metabolite rapidly reach comparable brainconcentrations within 1 hour, despite a lower plasma concentrationof the metabolite.

Key Words: glutamates • N-methyl-D-aspartate • neuroprotection • remacemide

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