CALPAIN INHIBITOR AK295 PROTECTS NEURONS FROM FOCAL BRAIN ISCHEMIA - EFFECTS OF POSTOCCLUSION INTRAARTERIAL ADMINISTRATION

被引：175

作者：

BARTUS, RT

HAYWARD, NJ

ELLIOTT, PJ

SAWYER, SD

BAKER, KL

DEAN, RL

AKIYAMA, A

STRAUB, JA

HARBESON, SL

LI, Z

POWERS, J

机构：

[1] TUFTS UNIV,DEPT PHARMACOL & EXPTL THERAPEUT,BOSTON,MA

[2] FOCAL INC,CAMBRIDGE,MA

[3] GEORGIA INST TECHNOL,ATLANTA,GA

来源：

STROKE | 1994年 / 25卷 / 11期

关键词：

CALCIUM; CALPAIN; CEREBRAL ISCHEMIA; RATS; NEUROPROTECTION;

D O I：

10.1161/01.STR.25.11.2265

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Background and Purpose This research was performed to determine whether a selective inhibitor of the calcium-depen dent protease, calpain, could reduce ischemia-associated brain damage when peripherally administered after a vascular occlusion. Methods A variation of the rat middle cerebral artery occlusion model was used. A range of doses of AK295 (a novel calpain inhibitor synthesized for this purpose) was continuously infused through the internal carotid artery, beginning 1.25 hours from the initiation of the occlusion. Rats were killed at 21 hours, and the infarct volume was quantified. Results Postocclusion (1.25-hour) infusion of the calpain inhibitor AK295 elicited a dose-dependent neuroprotective effect after focal ischemia. The highest dose tested (3 mg/kg per hour) afforded the maximum effect, illustrated by a 32% reduction in infarct volume 21 hours after the ischemia (vehicle, 81.7+/-4.7 mm(3); AK295, 54.9+/-6.9 mm(3); P<.007). Conclusions These data provide the first evidence that a peripherally administered calpain inhibitor can protect against ischemic brain damage. They offer further support for an important role of calpain proteolysis in the brain degeneration associated with cerebral ischemic events and suggest that selective calpain inhibitors provide a rational, novel, and viable means of treating such neurodegenerative problems.

引用

页码：2265 / 2270

页数：6

共 23 条

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