Attenuated hippocampal damage after global cerebral ischemia in mice mutant in neuronal nitric oxide synthase

被引：142

作者：

Panahian, N

Yoshida, T

Huang, PL

HedleyWhyte, ET

Dalkara, T

Fishman, MC

Moskowitz, MA

机构：

[1] HARVARD UNIV, MASSACHUSETTS GEN HOSP,SCH MED,DEPT SURG, STROKE & NEUROVASC REGULAT SECT NEUROSU, BOSTON, MA 02129 USA

[2] HARVARD UNIV, MASSACHUSETTS GEN HOSP,SCH MED,DEPT MED, DEPT NEUROL, BOSTON, MA 02129 USA

[3] HARVARD UNIV, MASSACHUSETTS GEN HOSP,SCH MED,DEPT MED, CARDIOVASC RES CTR, BOSTON, MA 02129 USA

[4] HARVARD UNIV, MASSACHUSETTS GEN HOSP, SCH MED, DEPT PATHOL, BOSTON, MA 02129 USA

来源：

NEUROSCIENCE | 1996年 / 72卷 / 02期

关键词：

global ischemia; nitric oxide; neurotoxicity; neuronal NOS gene;

D O I：

10.1016/0306-4522(95)00563-3

中图分类号：

Q189 [神经科学];

学科分类号：

071006 ;

摘要：

To address the importance of nitric oxide or its reaction products as mediators of neurotoxicity in brain, tissue injury was assessed after transient global ischemia in mice rendered mutant in the gene for neuronal nitric oxide synthase. Halothane-anesthetized wild type and mutant mice were subjected to temporary occlusion of the basilar plus both carotid arteries for 5 or 10 min followed by three days of reperfusion. Hippocampal injury, assessed both by qualitative grading and by cell counting in the CA1 subregion, was Significantly less in the mutant mice group after 5 or 10 min of ischemia. Mutant mice exhibited a lower mortality (P < 0.01), less weight loss, more normal grooming and spontaneous motor activity and better grasping in the 10 min group. There were no obvious differences in cerebrovascular anatomy or hemodynamics between wild type and mutant mice. The data suggest that a deficiency of neuronal nitric oxide synthase confers increased resistance to transient global cerebral ischemia, and support the suggestion that selective neuronal nitric oxide synthase inhibitors might reduce tissue injury associated with global cerebral ischemia.

引用

页码：343 / 354

页数：12

共 72 条

[51] ENDOTHELIAL NOS AND THE BLOCKADE OF LTP BY NOS INHIBITORS IN MICE LACKING NEURONAL NOS [J].

ODELL, TJ ;

HUANG, PL ;

DAWSON, TM ;

DINERMAN, JL ;

SNYDER, SH ;

KANDEL, ER ;

FISHMAN, MC .

SCIENCE, 1994, 265 (5171) :542-546

[52] THE ADENOSINE KINASE INHIBITOR, 5-IODOTUBERCIDIN, IS NOT PROTECTIVE AGAINST CEREBRAL ISCHEMIC-INJURY IN THE GERBIL [J].

PHILLIS, JW ;

SMITHBARBOUR, M .

LIFE SCIENCES, 1993, 53 (06) :497-502

[53] NEW MODEL OF BILATERAL HEMISPHERIC ISCHEMIA IN THE UNANESTHETIZED RAT [J].

PULSINELLI, WA ;

BRIERLEY, JB .

STROKE, 1979, 10 (03) :267-272

[54] TEMPORAL PROFILE OF NEURONAL DAMAGE IN A MODEL OF TRANSIENT FOREBRAIN ISCHEMIA [J].

PULSINELLI, WA ;

BRIERLEY, JB ;

PLUM, F .

ANNALS OF NEUROLOGY, 1982, 11 (05) :491-498

[55] A CRYOPROTECTION METHOD THAT FACILITATES CUTTING FROZEN-SECTIONS OF WHOLE MONKEY BRAINS FOR HISTOLOGICAL AND HISTOCHEMICAL PROCESSING WITHOUT FREEZING ARTIFACT [J].

ROSENE, DL ;

ROY, NJ ;

DAVIS, BJ .

JOURNAL OF HISTOCHEMISTRY & CYTOCHEMISTRY, 1986, 34 (10) :1301-1315

[56] NITRIC-OXIDE INHIBITION AGGRAVATES ISCHEMIC DAMAGE OF HIPPOCAMPAL BUT NOT OF NADPH NEURONS IN GERBILS [J].

SANCESARIO, G ;

IANNONE, M ;

MORELLO, M ;

NISTICO, G ;

BERNARDI, G .

STROKE, 1994, 25 (02) :436-443

[57]

SIDMAN RL, 1971, ATLAS MOUSE BRAIN SP, P44

[58] NEUROCYTOTOXICITY - PHARMACOLOGICAL IMPLICATIONS [J].

SIESJO, BK ;

MEMEZAWA, H ;

SMITH, ML .

FUNDAMENTAL & CLINICAL PHARMACOLOGY, 1991, 5 (09) :755-767

[59] CALCIUM FLUXES, CALCIUM-ANTAGONISTS, AND CALCIUM-RELATED PATHOLOGY IN BRAIN ISCHEMIA, HYPOGLYCEMIA, AND SPREADING DEPRESSION - A UNIFYING HYPOTHESIS [J].

SIESJO, BK ;

BENGTSSON, F .

JOURNAL OF CEREBRAL BLOOD FLOW AND METABOLISM, 1989, 9 (02) :127-140

[60] MODELS FOR STUDYING LONG-TERM RECOVERY FOLLOWING FOREBRAIN ISCHEMIA IN THE RAT .2. A 2-VESSEL OCCLUSION MODEL [J].

SMITH, ML ;

BENDEK, G ;

DAHLGREN, N ;

ROSEN, I ;

WIELOCH, T ;

SIESJO, BK .

ACTA NEUROLOGICA SCANDINAVICA, 1984, 69 (06) :385-401

← 1 2 3 4 5 6 7 8 →