2010
DOI: 10.1097/fjc.0b013e3181c5e7d4
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Cardiovascular Effects of Oxytocin Infusion in a Porcine Model of Myocardial Infarct

Abstract: The effects of oxytocin (OT) on cardiovascular endpoints were assessed in a myocardial infarct (MI) model. OT (10 ng.kg(-1).hour(-1)) or saline infusion was initiated at reperfusion (D0) or 8 days (D8) after MI. Our hypothesis was that OT administration to individuals with a low pretreatment OT levels (PTOT) may be beneficial, whereas individuals with an elevated PTOT would be prone to adverse effects. Starting OT on D0 reduced left ventricular fraction shortening evaluated 8 days post MI and had no effect on … Show more

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Cited by 14 publications
(12 citation statements)
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“…OT administration to individuals with a low pretreatment OT levels could be beneficial whereas, individuals with an elevated basal OT levels would be prone to adverse effects, which has been shown in swine (Jacquenod et al, 2015). It is likely that during parturition the basal OT levels are already very high, a bolus injection of OT in large amount may reversely decrease OTR signaling by reducing OTR protein expression (Authier et al, 2010). Moreover, high doses of OT also activated VP receptors (Wang and Hatton, 2006), thereby evoking MI (Ying et al, 2015).…”
Section: Limitation For Therapeutic Use Of Otmentioning
confidence: 99%
“…OT administration to individuals with a low pretreatment OT levels could be beneficial whereas, individuals with an elevated basal OT levels would be prone to adverse effects, which has been shown in swine (Jacquenod et al, 2015). It is likely that during parturition the basal OT levels are already very high, a bolus injection of OT in large amount may reversely decrease OTR signaling by reducing OTR protein expression (Authier et al, 2010). Moreover, high doses of OT also activated VP receptors (Wang and Hatton, 2006), thereby evoking MI (Ying et al, 2015).…”
Section: Limitation For Therapeutic Use Of Otmentioning
confidence: 99%
“…Finally, downregulation of the OT system is associated with dilated cardiomyopathy [ 83 ], hypertension [ 84 ] and impaired cardiovascular function [ 19 , 46 , 68 , 80 ]. In a porcine myocardial infarct model, placebo-treated animals with high endogenous OT levels at the start of the experiment had better ejection fraction overall compared to OT-treated animals with high basal endogenous OT levels [ 85 ]. In contrast, in the low endogenous OT group receiving exogenous OT had no effect on cardiac function or cardiac OTR expression [ 85 ], yet the group with low basal OT levels without OT treatment had reduced function and larger infarct size [ 85 ].…”
Section: Ot/otr In Cardiac and Vascular Protectionmentioning
confidence: 99%
“…In a porcine myocardial infarct model, placebo-treated animals with high endogenous OT levels at the start of the experiment had better ejection fraction overall compared to OT-treated animals with high basal endogenous OT levels [ 85 ]. In contrast, in the low endogenous OT group receiving exogenous OT had no effect on cardiac function or cardiac OTR expression [ 85 ], yet the group with low basal OT levels without OT treatment had reduced function and larger infarct size [ 85 ]. Thus, the potential of OT to exert its cardio-protective effects seems to be at least in part dependent on the presence of both its basal receptor and its ligand.…”
Section: Ot/otr In Cardiac and Vascular Protectionmentioning
confidence: 99%
“…In rat, rabbit and pig models of ischemic heart disease, OT treatment significantly reduced infarct size and improved parameters of heart function [28,29,30,31]. …”
Section: Cardiac Ot Actionsmentioning
confidence: 99%