Microplasmin: A Novel Thrombolytic That Improves Behavioral Outcome After Embolic Strokes in Rabbits

doi:10.1161/01.STR.0000028267.09604.7B

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Stroke. 2002;33:2279-2284
doi: 10.1161/01.STR.0000028267.09604.7B

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	Thrombolysis
	Acute Cerebral Hemorrhage
	Acute Cerebral Infarction
	Embolic stroke

(Stroke. 2002;33:2279.)
© 2002 American Heart Association, Inc.

Original Contributions

Microplasmin: A Novel Thrombolytic That Improves Behavioral Outcome After Embolic Strokes in Rabbits

Paul A. Lapchak, PhD; Dalia M. Araujo, PhD; Steve Pakola, MD; Donghuan Song, MD; Jiandong Wei, MD Justin A. Zivin, MD, PhD

From the Department of Neuroscience, University of California at San Diego, La Jolla (P.A.L., D.S., J.W., J.A.Z.); VA San Diego Healthcare System, San Diego, Calif (P.A.L., D.M.A., D.S., J.W., J.A.Z.); Veterans Medical Research Foundation, San Diego, Calif (P.A.L., D.S., J.W., J.A.Z.); and ThromboGenics Ltd, Dublin, Ireland (S.P.).

Correspondence to Dr Paul A. Lapchak, Department of Neuroscience, University of California at San Diego, MTF 316, 9500 Gilman Dr, La Jolla, CA 92093-0624. E-mail plapchak{at}ucsd.edu

Background and Purpose— It has been proposed that thenovel thrombolytic microplasmin may be useful in the treatmentof ischemic stroke. In the present study the effects and safetyprofile of microplasmin were evaluated in 2 rabbit embolic strokemodels that have been used successfully to develop tissue plasminogenactivator (tPA) as the only Food and Drug Administration-approvedtreatment for stroke. The rabbit small clot embolic stroke model(RSCEM) and rabbit large clot embolic stroke model (RLCEM) wereused to determine the potential neuroprotective properties andsafety profile of microplasmin, respectively, after an embolicstroke.

Methods— Rabbits were embolized by injecting small bloodclots (RSCEM) or large blood clots (RLCEM) into the cerebralcirculation. For the RSCEM, 126 rabbits were included, withbehavioral analysis conducted 24 hours later, allowing for determinationof the effective stroke dose (ES₅₀) or clot amount (milligrams)that produces severe neurological deficits in 50% of rabbits.For RLCEM safety study analysis, 47 rabbits were included, withpostmortem analyses consisting of assessment of hemorrhage andinfarct rate and size. In test animals microplasmin was infusedintravenously 60 minutes after embolization, whereas controlrabbits were given infusions of the saline/Plasma-Lyte vehiclewith all assessments performed in a blinded fashion.

Results— In the RSCEM, a drug is considered neuroprotectiveif it significantly increases the ES₅₀ compared with the vehicle-treatedcontrol group. The ES₅₀ of the vehicle-treated control group24 hours after embolization was 1.36±0.42 mg (n=38).Microplasmin, infused starting 60 minutes after embolization,increased the ES₅₀ to 2.32±0.57 (n=21), 1.89±0.48(n=21), 2.81±0.55 (n=22), and 1.89±0.28 mg (n=24)for the 1-, 2-, 4-, and 8-mg/kg doses, respectively. There wasa statistically significant behavioral improvement in the 4-mg/kgdose arm (P=0.040). The microplasmin dose of microplasmin thatwas statistically significant (4 mg/kg) was subsequently determinedto be safe in the RLCEM because it did not increase the incidenceof hemorrhages (56%) compared with vehicle-treated rabbits (63%),nor did it significantly alter hemorrhage volume, infarct rate,or infarct volume.

Conclusions— The present study shows that microplasminimproves behavioral rating scores in the RSCEM when administered60 minutes after embolization, at a dose that does not increasehemorrhages in the RLCEM. This is in contrast to tPA, whichsignificantly enhances the hemorrhage rate in the RLCEM.

Key Words: ischemia • neuroprotection • reperfusion • thrombolytic therapy • tissue plasminogen activator • rabbits

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