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Research Article Free access | 10.1172/JCI107511

Mechanisms Regulating the Cardiac Output Response to Cyanide Infusion, a Model of Hypoxia

Chang-seng Liang and William E. Huckabee

Department of Medicine, Boston University School of Medicine, Boston, Massachusetts 02118

Department of Pharmacology, Boston University School of Medicine, Boston, Massachusetts 02118

Department of Medicine, University Hospital, Boston, Massachusetts 02118

Department of Clinical Research, University Hospital, Boston, Massachusetts 02118

Find articles by Liang, C. in: PubMed | Google Scholar

Department of Medicine, Boston University School of Medicine, Boston, Massachusetts 02118

Department of Pharmacology, Boston University School of Medicine, Boston, Massachusetts 02118

Department of Medicine, University Hospital, Boston, Massachusetts 02118

Department of Clinical Research, University Hospital, Boston, Massachusetts 02118

Find articles by Huckabee, W. in: PubMed | Google Scholar

Published December 1, 1973 - More info

Published in Volume 52, Issue 12 on December 1, 1973
J Clin Invest. 1973;52(12):3115–3128. https://doi.org/10.1172/JCI107511.
© 1973 The American Society for Clinical Investigation
Published December 1, 1973 - Version history
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Abstract

When tissue metabolic changes like those of hypoxia were induced by intra-aortic infusion of cyanide in dogs, cardiac output began to increase after 3 to 5 min, reached a peak (220% of the control value) at 15 min, and returned to control in 40 min. This pattern of cardiac output rise was not altered by vagotomy with or without atropine pretreatment. However, this cardiac output response could be differentiated into three phases by pretreating the animals with agents that block specific activities of the sympatho-adrenal system. First, ganglionic blockade produced by mecamylamine or sympathetic nerve blockade by bretylium abolished the middle phase of the cardiac output seen in the untreated animal, but early and late phases still could be discerned. Second, beta-adrenergic receptor blockade produced by propranolol shortened the total duration of the cardiac output rise by abolishing the late phase. Third, when given together, propranolol and mecamylamine (or bretylium) prevented most of the cardiac output rise that follows the early phase.

When cyanide was given to splenectomized dogs, the duration of the cardiac output response was not shortened, but the response became biphasic, resembling that seen after chemical sympathectomy. A similar biphasic response of the cardiac output also resulted from splenic denervation; sham operation or nephrectomy had no effect on the monophasic pattern of the normal response. Splenic venous blood obtained from cyanide-treated dogs, when infused intraportally, caused an increase in cardiac output in recipient dogs; similar infusion of arterial blood had no effects.

These results suggest that the cardiac output response to cyanide infusion consists of three components: an early phase, related neither to the autonomic nervous system nor to circulating catecholamines; a middle phase, caused by a nonadrenergic humoral substance released from the spleen by sympathetic stimulation; and a late phase, dependent upon adrenergic receptors but not upon sympathetic transmission.

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