Comparative Cardiac Effects of Terlipressin, Vasopressin, and Norepinephrine on an Isolated Perfused Rabbit Heart |
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Authors: | Ouattara, Alexandre M.D. Landi, Marc M.D. Le Manach, Yannick M.D. Lecomte, Patrick M.D. Leguen, Morgan M.D. Boccara, Gilles M.D., Ph.D. Coriat, Pierre M.D. Riou, Bruno M.D., Ph.D.
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Affiliation: | Ouattara, Alexandre M.D.*; Landi, Marc M.D.*; Le Manach, Yannick M.D.†; Lecomte, Patrick M.D.†; Leguen, Morgan M.D.†; Boccara, Gilles M.D., Ph.D.*; Coriat, Pierre M.D.‡; Riou, Bruno M.D., Ph.D.§ |
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Abstract: | Background: Terlipressin, a synthetic analog of arginine-vasopressin (AVP), has been proposed as an effective vasopressive therapy in catecholamine-resistant vasodilatory shock. Although beneficial effects of terlipressin on systemic arterial pressure have been clearly demonstrated, its intrinsic effects on coronary circulation and myocardial performances remain unknown. Methods: The authors compared the coronary and myocardial effects of terlipressin (1-100 nm, n = 10), AVP (10-1000 pm, n = 10), and norepinephrine (1-100 nm, n = 10) on an erythrocyte-perfused isolated rabbit heart. The cardiac effects of terlipressin were also assessed in erythrocyte-perfused hearts in which the myocardial oxygen delivery was maintained constant and buffer-perfused hearts. Finally, the cardiac effects of terlipressin and AVP were studied in hearts pretreated by [d(CH2)5Tyr(Me)]AVP (0.1 [mu]m), a selective V1a receptor antagonist. Results: Norepinephrine induced a biphasic coronary effect associated with a concentration-dependent increase in myocardial performances. AVP and terlipressin significantly decreased coronary blood flow and impaired myocardial performances from 30 pm and 30 nm, respectively (P < 0.05). The cardiac side-effects of terlipressin were confirmed in buffer-perfused hearts but the maintenance of a constant myocardial oxygen delivery constant abolished its effects on myocardial performances. The cardiac effects induced by terlipressin and AVP were nearly completely abolished on hearts pretreated by [d(CH2)5Tyr(Me)]AVP. |
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