Abstract

Although the pathophysiologic response of the brain to a reduced oxygen availability has been studied for many years the exact mechanism by which cerebral damage is incurred is not known. It is also unclear whether the mechanism of damage is the same for ischemia (a reduction in cerebral blood flow) and hypoxia (a reduction in blood oxygen content). The overall goals of this project are to clarify the role of oxygen derived free radical mechanisms in the pathophysiology of global cerebral ischemia and hypoxia and to determine if the apparent ability of newborn animals to tolerate reduced cerebral oxygen availability is related to a free radical mechanism. We hypothesize that increasing the duration of an ischemic insult is associated with decreased recovery of post ischemic cerebral blood flow and oxygen consumption, decreased post ischemic recovery of neurologic function and increased post ischemic production of oxygen derived free radicals, but that these changes will be less marked in newborns. Likewise, we hypothesize that there will be an increased release of oxygen derived free radicals during reoxygenation after pure hypoxia. Ischemia will be induced by cross clamping the ascending aorta after occlusion of the vena cavae. In both newborn and older animals ischemia will be maintained for variable times to determine whether changing the interval of ischemia or the administration of oxygen derived free radical scavengers (e.g. superoxide dismutase) has an effect on post ischemic sequela. The variables that will be measured include cerebral blood flow (radiolabelled microsphere technique), cerebral oxygen consumption (Fick principle), cerebral function (evoked potentials) and production of oxygen derived free radicals (nitroblue-tetrazolium technique). Cerebral hypoxia will be produced by lowering the inspired oxygen content while maintaining arterial PCO2 and pH normal. In this group of animals hypoxia will be maintained at one of two levels (5% or 10% O2) for ten minutes and the rate of free radical production will be determined during reoxygenation. From our data we will be able to determine whether oxygen derived free radical mechanisms are associated with cerebral ischemia or hypoxia.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Clinical Investigator Award (CIA) (K08)
Project #
5K08NS001225-02
Application #
3084029
Study Section
Neurological Disorders Program Project Review A Committee (NSPA)
Project Start
1987-08-01
Project End
1992-07-31
Budget Start
1988-08-01
Budget End
1989-07-31
Support Year
2
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Cheng, W; Hartmann, J F; Cameron, D E et al. (1995) Cerebral blood flow during cardiopulmonary bypass: influence of temperature and pH management strategy. Ann Thorac Surg 59:880-6
Ulatowski, J A; Kirsch, J R; Traystman, R J (1994) Hypoxic reperfusion after ischemia in swine does not improve acute brain recovery. Am J Physiol 267:H1880-7
Clavier, N; Kirsch, J R; Hurn, P D et al. (1994) Cerebral blood flow is reduced by N omega-nitro-L-arginine methyl ester during delayed hypoperfusion in cats. Am J Physiol 267:H174-81
Nishikawa, T; Kirsch, J R; Koehler, R C et al. (1994) Nitric oxide synthase inhibition reduces caudate injury following transient focal ischemia in cats. Stroke 25:877-85
Moore, L E; Kirsch, J R; Helfaer, M A et al. (1994) Nitric oxide and prostanoids contribute to isoflurane-induced cerebral hyperemia in pigs. Anesthesiology 80:1328-37
Ichord, R N; Helfaer, M A; Kirsch, J R et al. (1994) Nitric oxide synthase inhibition attenuates hypoglycemic cerebral hyperemia in piglets. Am J Physiol 266:H1062-8
Hoehner, P J; Kirsch, J R; Helfaer, M A et al. (1994) Dihydropyridine ligand binding decreases earlier in adolescent than in infant swine after global cerebral ischemia. Stroke 25:2060-5;discussion 2066
Greenberg, R S; Helfaer, M A; Kirsch, J R et al. (1994) Nitric oxide synthase inhibition with NG-mono-methyl-L-arginine reversibly decreases cerebral blood flow in piglets. Crit Care Med 22:384-92
Takeshima, R; Kirsch, J R; Koehler, R C et al. (1994) Tirilazad treatment does not decrease early brain injury after transient focal ischemia in cats. Stroke 25:670-6
Diringer, M N; Kirsch, J R; Traystman, R J (1994) Reduced cerebral blood flow but intact reactivity to hypercarbia and hypoxia following subarachnoid hemorrhage in rabbits. J Cereb Blood Flow Metab 14:59-63

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