NITRIC-OXIDE PROMOTES ARTERIOLAR DILATION DURING CORTICAL SPREADING DEPRESSION IN RABBITS

被引：48

作者：

COLONNA, DM

MENG, W

DEAL, DD

BUSIJA, DW

机构：

[1] WAKE FOREST UNIV,BOWMAN GRAY SCH MED,DEPT PHYSIOL & PHARMACOL,CARDIOVASC PROGRAMS,WINSTON SALEM,NC 27103

[2] WAKE FOREST UNIV,BOWMAN GRAY SCH MED,DEPT PHYSIOL & PHARMACOL,PROGRAM NEUROSCI,WINSTON SALEM,NC 27103

来源：

STROKE | 1994年 / 25卷 / 12期

关键词：

NITRIC OXIDE; SPREADING CORTICAL DEPRESSION; RABBITS;

D O I：

10.1161/01.STR.25.12.2463

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 Pial arterioles transiently dilate during cortical spreading depression (CSD), although the mechanisms are unclear. We tested the hypothesis that increased production of nitric oxide (NO) promotes arteriolar dilation. Methods Urethane-anesthetized rabbits were equipped with cranial windows, and the diameter (reported in micrometers) of a pial arteriole was determined via intravital microscopy. In each rabbit, a baseline CSD was elicited by microapplication of KCl onto the cortex, and resultant pial arteriolar dilation was measured. Either 100 mu mol/L N-omega-nitro-L-arginine methyl ester (L-NAME) or 50 mu mol/L N-G-nitro-L-arginine (L-NA), both competitive NO synthase inhibitors, was then applied to the brain surface. A CSD was elicited as before. The L-NAME and L-NA were then removed by artificial cerebrospinal fluid washes. An additional CSD was induced with KCl as before. Results Control CSD in the L-NAME group dilated pial arterioles: baseline diameter, 66+/-7 mm, with CSD=106+/-8 mm (59% increase). After topically applied L-NAME, CSD dilated pial arterioles less: baseline diameter, 61+/-7 mm, with CSD=77+/-6 mm (26% increase), P < .05 compared with control CSD diameter. Topical L-NA had similar effects on CSD: control CSD dilated pial arterioles 51%; after topical L-NA, only 14% (P<.05). After removal of L-NAME or L-NA, CSD-induced pial arteriolar dilation was similar to original control values. Conclusions The reversible inhibition of CSD-induced pial arteriolar dilation by either L-NAME or L-NA suggests that NO contributes to arteriolar dilation observed with CSD.

引用

页码：2463 / 2470

页数：8

共 38 条

[11] EXAMINATION OF THE ROLE OF NITRIC-OXIDE FOR THE HYPERCAPNIC RISE OF CEREBRAL BLOOD-FLOW IN RATS [J].

FABRICIUS, M ;

LAURITZEN, M .

AMERICAN JOURNAL OF PHYSIOLOGY, 1994, 266 (04) :H1457-H1464

[12] NITRIC-OXIDE MEDIATES VASODILATATION IN RESPONSE TO ACTIVATION OF N-METHYL-D-ASPARTATE RECEPTORS IN BRAIN [J].

FARACI, FM ;

BREESE, KR .

CIRCULATION RESEARCH, 1993, 72 (02) :476-480

[13] EFFECT OF ADENOSINE ON CALCIUM-UPTAKE BY INTACT AND CULTURED VASCULAR SMOOTH-MUSCLE [J].

FENTON, RA ;

BRUTTIG, SP ;

RUBIO, R ;

BERNE, RM .

AMERICAN JOURNAL OF PHYSIOLOGY, 1982, 242 (05) :H797-H804

[14] DIMINISHED ARTERIAL SMOOTH-MUSCLE RESPONSE TO ADENOSINE DURING NA-K PUMP INHIBITION [J].

FOLEY, DH .

PFLUGERS ARCHIV-EUROPEAN JOURNAL OF PHYSIOLOGY, 1984, 400 (01) :88-95

[15] ENDOTHELIUM-DERIVED RELAXING FACTOR RELEASE ON ACTIVATION OF NMDA RECEPTORS SUGGESTS ROLE AS INTERCELLULAR MESSENGER IN THE BRAIN [J].

GARTHWAITE, J ;

CHARLES, SL ;

CHESSWILLIAMS, R .

NATURE, 1988, 336 (6197) :385-388

[16] NITRIC-OXIDE SYNTHESIS COUPLES CEREBRAL BLOOD-FLOW AND METABOLISM [J].

GOADSBY, PJ ;

KAUBE, H ;

HOSKIN, KL .

BRAIN RESEARCH, 1992, 595 (01) :167-170

[17] EXTRACELLULAR ION CONCENTRATIONS DURING SPREADING DEPRESSION AND ISCHEMIA IN THE RAT-BRAIN CORTEX [J].

HANSEN, AJ ;

ZEUTHEN, T .

ACTA PHYSIOLOGICA SCANDINAVICA, 1981, 113 (04) :437-445

[18]

HANSEN AJ, 1988, NEUROL NEUR, V46, P661

[19] NITRIC-OXIDE SYNTHASE-CONTAINING NEURAL PROCESSES ON LARGE CEREBRAL-ARTERIES AND CEREBRAL MICROVESSELS [J].

IADECOLA, C ;

BEITZ, AJ ;

RENNO, W ;

XU, X ;

MAYER, B ;

ZHANG, F .

BRAIN RESEARCH, 1993, 606 (01) :148-155

[20] ANTIMIGRAINE COMPOUNDS FAIL TO MODULATE THE PROPAGATION OF CORTICAL SPREADING DEPRESSION IN THE CAT [J].

KAUBE, H ;

GOADSBY, PJ .

EUROPEAN NEUROLOGY, 1994, 34 (01) :30-35

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