ROLE OF NA+/PHOSPHATE-COTRANSPORTER IN MYOCARDIAL CONTRACTILE RESPONSES TO ALPHA(1)-AGONIST

被引:3
作者
ONWOCHEI, MO
机构
[1] Department of Pharmacology and Therapeutics, Medical College of Ohio, Toledo, OH
关键词
INORGANIC PHOSPHATE; RAT HEART; PHOSPHONOFORMATE; ADRENERGIC AGENTS; PHOSPHOINOSITIDE PATHWAY; MYOCARDIAL CONTRACTILITY;
D O I
10.1097/00005344-199505000-00021
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
The interaction of cardiac sodium/phosphate (Na+/Pi)-cotransporter and the phosphoinositide pathway (PIP) in influencing myocardial contraction was investigated. Specifically, the study was performed to determine if myocardial positive inotropic response (+dP/dt) to phenylephrine (PE, an activator of PIP) can be potentiated by inorganic phosphate (Pi, the substrate of Na+/Pi-cotransporter). Contractile responses of the isolated perfused rat heart were studied in conditions of controlled extracellular calcium activity and constant preload. The data showed that phenylephrine-induced increase in +dP/dt was potentiated by Pi. Prazosin inhibited this increase in +dP/dt, indicating alpha(1)-adrenergic involvement. This Pi-potentiated increase in +dP/dt was also inhibited by phosphonoformate (PFA); however, only partial inhibition was obtained with concentrations of PFA that selectively inhibited Na+/Pi-cotransporter. Isoproterenol-induced increase in +dP/dt was not potentiated by Pi, showing that potentiation of +dP/dt is not a common effect of Pi. The data support an important interaction between PIP and Na+/Pi-cotransporter in regulating myocardial contraction.
引用
收藏
页码:833 / 839
页数:7
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