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J Thorac Cardiovasc Surg 1996;112:698-707
© 1996 Mosby, Inc.

SURGERY FOR CONGENITAL HEART DISEASE

CEREBRAL METABOLIC RECOVERY FROM DEEP HYPOTHERMIC CIRCULATORY ARREST AFTER TREATMENT WITH ARGININE AND NITRO-ARGININE METHYL ESTER

Takeshi Hiramatsu, MDa, Richard A. Jonas, MDa, Takuya Miura, MDa, Adre duPlessis, MDb, Masahiro Tanji, MDa, Joseph M. Forbess, MDa, David Holtzman, MD, PhDb

Funded by a National Institutes of Health Resource Grant (RR-00995) and the Research Fund of the Department of Cardiac Surgery (Children's Hospital).

Received for publication Feb. 6, 1996 Revisions requested March 6, 1996; revisions received April 3, 1996 Accepted for publication April 4, 1996. Address for reprints: Richard A. Jonas, MD, Department of Cardiac Surgery, Children's Hospital, 300 Longwood Ave., Boston, MA 02115.

Abstract

Background: Recent studies suggest that nitric oxide is important in the pathogenesis of ischemic brain injury and also has a role in controlling cerebrovascular tone. This study examines the net effects of nitric oxide on cerebral metabolic recovery after deep hypothermic circulatory arrest. Methods: Two-week-old piglets were supported by cardiopulmonary bypass and cooled to 15º C followed by 1 hour of deep hypothermic circulatory arrest, 45 minutes of reperfusion and rewarming, and then 3 hours of normothermic perfusion. Groups of 10 piglets received one of four treatments before bypass: L-nitro-arginine methyl ester, inhibitor of nitric oxide synthesis, 10 mg/kg intravenously; L-arginine, to enhance nitric oxide synthesis, 30 mg/kg intravenously before bypass and then 10 mg/kg per minute during the first hour of reperfusion; a combination of L-nitro-arginine methyl ester plus L-arginine at these same doses; and no pretreatment (controls). Cerebral high-energy phosphates and pH were measured by magnetic resonance spectroscopy in half the animals. Cerebral blood flow, metabolic rates for oxygen and glucose, and the oxidation/reduction state of cytochrome aa3 and oxygenated and deoxygenated hemoglobin measured by near-infrared spectroscopy were assessed in the other half of the piglets. Results: L-nitro-arginine methyl ester significantly increased cerebral vascular resistance and markedly reduced recovery of high-energy phosphates, pH, and oxidation state of cytochrome aa3. L-arginine increased cerebral blood flow, cerebral glucose and oxygen consumption, and recovery of cytochrome aa3 oxidation and high-energy phosphates. L-Arginine did not reverse completely the effects of L-nitro-arginine methyl ester on cerebral metabolic recovery. Conclusion: In a piglet model of deep hypothermic circulatory arrest, L-nitro-arginine methyl ester has a deleterious effect and L-arginine has a beneficial effect on cerebral metabolic recovery. The deleterious metabolic effects of L-nitro-arginine methyl ester are only partially reversed by L-arginine. This fact suggests that there may be mechanisms in addition to inhibition of nitric oxide synthesis contributing to the neurotoxicity of L-nitro-arginine methyl ester in this model. (J THORAC CARDIOVASC SURG 1996;112:698-707)




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