Roles of the Sarcoplasmic/Endoplasmic Reticulum Ca2+-ATPase, Plasma Membrane Ca2+-ATPase and Na+/Ca2+ Exchanger in Regulation of Heart Rate in Larval Drosophila

Mohati Desai-Shah, A. Papoy, M. Ward, R. Cooper
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引用次数: 37

Abstract

We investigated the roles of three regulatory proteins that impact [Ca 2+ ]i within cardiac myocytes of Drosophila melanogaster. The NCX (Na + /Ca 2+ exchanger), PMCA (plasma membrane Ca 2+ -ATPase) and SERCA (sarcoplasmic/endoplasmic reticulum Ca 2+ -ATPase) were compromised by ionic, pharmacological, mutationalmanipulation, and with a combination of approaches, while heart rate (HR) was monitored. A decrease in SERCA function reduced HR more for intact larva in comparison to a dissected larva. Dissected preparations were used to expose the heart directly to agents. A compromised PMCA also reduced HR; however, attenuated NCX function by low [Na + ]o increased HR. KBR7943, a blocker of Ca 2+ entry via NCX, exposure increased HR. A combined loss of function in all three channels did not show a significant change in HR. The results indicate that NCX and PMCA are important in regulating HR, whereas SERCA does not have as pronounced role for dissected preparations. However, with intact preparations the loss of SERCA function by a mutation does have a significant impact on HR. Pharmacological approaches to alter PMCA and SERCA paralleled the results obtained by ionic and mutational approaches. To further understand the pacemaker activity, intracellular recordings were obtained. Mapping of action-potentials in myocytes revealed that the caudal region of the heart has large amplitude potentials and is likely to contain the pacemaker cells. The Drosophila heart can serve as a genetic model in understanding regulation of ionic currents for pacing cells of various types.
肌浆/内质网Ca2+- atp酶、质膜Ca2+- atp酶和Na+/Ca2+交换器在果蝇幼虫心率调节中的作用
我们研究了影响黑腹果蝇心肌细胞[ca2 +]i的三种调节蛋白的作用。NCX (Na + / ca2 +交换器)、PMCA(质膜ca2 + - atp酶)和SERCA(肌浆/内质网ca2 + - atp酶)被离子、药理学、突变操作和多种方法联合破坏,同时监测心率(HR)。与解剖后的幼虫相比,完整幼虫SERCA功能的降低更能降低HR。使用解剖的制剂将心脏直接暴露于药剂中。PMCA受损也会降低HR;然而,低[Na +]降低NCX功能或增加HR。KBR7943是一种Ca 2+通过NCX进入的阻断剂,暴露会增加HR。三个通道功能的综合丧失在HR中没有显示出显著的变化。结果表明NCX和PMCA在调节HR方面很重要,而SERCA在解剖制剂中没有明显的作用。然而,在完整的制备中,突变导致SERCA功能的丧失确实会对HR产生重大影响。改变PMCA和SERCA的药理学方法与离子和突变方法获得的结果相似。为了进一步了解起搏器的活动,我们获得了细胞内的记录。肌细胞的动作电位图显示,心脏尾侧区域具有大振幅电位,可能包含起搏器细胞。果蝇心脏可以作为一种遗传模型来理解各种类型起搏细胞的离子电流调节。
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