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2003 Fiscal Year Final Research Report Summary

Pharmacologic evaluation of protective efficacy of caspase inhibitor, diazoxide for spinal cord protection using aspartate segmental infusion model. -Strategy against paraplegia by reducing mitochondrial-dependent apoptotic pathway

Research Project

Project/Area Number 14571276
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeSingle-year Grants
Section一般
Research Field Thoracic surgery
Research InstitutionKEIO UNIVERSITY

Principal Investigator

SHIMIZU Hideyuki  Keio University, School of Medicine, Instructor, 医学部, 助手 (50226247)

Project Period (FY) 2002 – 2003
KeywordsAspartate / Delayed onset paraplegia / Diazoxide / Caspase inhibitor / NMDA / Experimental model / Spinal cord protection / Aspartate segmental infusion model
Research Abstract

We evaluated the protective effects of caspase inhibitor, diazoxide on spinal cord neurons using segmental aspartate infusion model under brief ischemia in vivo. New Zealand white rabbits underwent an infrarenal aortic isolation. Group A animals(n=7) received intravenous pretreatment of caspase inhibitor, diazoxide (4mg/kg). Group B animals(n=7) received pretreatment of NMDA antagonist, MK-801(6mg/kg) after the pretreatment similar to group A. Group C animals (n=7) received oral medication of riluzole(100mg/kg/day) preoperatively for ten days adding the pretreatment similar to group A. Group D animals(n=7) received viehcles only as a control of group A. Animals received segmental aspartate(30 mM) infusion for 10 minutes at a rate of 2ml/min. Neurologic status was scored at 12,24 and 48 hours after surgery using Tarlov score. Neurologic status was 3.8±0.9 in group A, 3.4±0.6 in group B, 4.0±0.6 in group C, 0.8±0.6 in group D respectively. Animals in group A showed significantly better neurologic recovery compared with group D (p<0.05). There was no significant difference between the functional scores of group A, group Band groupC respectively. Sections from group D exhibited severe gray matter necrosis in ventral horn. In contrast, group A, group B and group C exhibited mild neuronal change with eosinophilic changes. Diazoxide might ameliorate the spinal cord injury induced by segmental aspartate infusion combined with brief ischemia. Pharmacologic strategy using caspase inhibitor, might be a promising strategy against delayed onset paraplegia associated with aortic surgery reducing aspartate excitotoxicity.

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Published: 2005-04-19  

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