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Potential
Role of Neuroprotective Agents in the Treatment of
Patients with Acute Ischemic Stroke.
Ovbiagele B, Kidwell CS, Starkman S, Saver JL.
Curr
Treat Options Cardiovasc Med. 2003 Dec;5(6):441-449.
Stroke
Center
and Department of Neurology, University
of California
at Los
Angeles,
710 Westwood Plaza, Los
Angeles,
CA
90095,
USA.
This e-mail address is being protected from spambots. You need JavaScript enabled to view it
Currently, intravenous
recombinant tissue plasminogen activator is the only
US Food and Drug Administration-approved therapy for acute ischemic stroke.
Although efficacious, its usefulness is limited, mainly because of the very
limited time window for its administration. Neuroprotective treatments are therapies that block the
cellular, biochemical, and metabolic elaboration of injury during or after
exposure to ischemia, and have a potential role in ameliorating brain injury in
patients with acute ischemic stroke. More than 50 neuroprotective agents have reached randomized human
clinical trials in focal ischemic stroke, but none have been unequivocally
proven efficacious, despite successful preceding animal studies. The failed
neuroprotective trials of the past have greatly
increased understanding of the fundamental biology of ischemic brain injury and
have laid a strong foundation for future advance. Moreover, the recent favorable results of human clinical trials of hypothermia in
human cardiac arrest and global brain ischemia have validated the general
concept of neuroprotection for ischemic brain injury.
Recent innovations in strategies of preclinical drug development and clinical
trial design that rectify past defects hold great promise for neuroprotective investigation, including novel approaches to
accelerating time to initiation of experimental treatment, use of outcome
measures sensitive to treatment effects, and trial testing of combination
therapies rather than single agents alone. Although no neuroprotective agent is of proven benefit for focal
ischemic stroke, several currently available interventions have shown promising
results in preliminary trials and may be considered for cautious, off-label use
in acute stroke, including hypothermia, magnesium sulfate, citicoline, albumin, and
erythropoietin. Overall, the prospects for safe and effective neuroprotective therapies to improve stroke outcome remain
promising.
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