TRPM7 silencing attenuates Mg2+ influx in cardiac myoblasts, H9c2 cells

被引:0
作者
Michiko Tashiro
Masato Konishi
Ryo Kobayashi
Hana Inoue
Utako Yokoyama
机构
[1] Tokyo Medical University,Department of Physiology
[2] Tokyo Medical University,Department of Microbiology
来源
The Journal of Physiological Sciences | 2020年 / 70卷
关键词
Magnesium; TRPM7; Cardiac myoblast; H9c2; Mag-fura-2;
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摘要
TRPM7, a member of the melastatin subfamily of transient receptor potential channels, is suggested to be a potential candidate for a physiological Mg2+ channel. However, there is no direct evidence of Mg2+ permeation through endogenous TRPM7. To determine the physiological roles of TRPM7 in intracellular Mg2+ homeostasis, we measured the cytoplasmic free Mg2+ concentration ([Mg2+]i) in TRPM7-silenced H9c2 cells. [Mg2+]i was measured in a cluster of 8–10 cells using the fluorescent indicator, furaptra. TRPM7 silencing did not change [Mg2+]i in Ca2+-free Tyrode’s solution containing 1 mM Mg2+. Increasing the extracellular Mg2+ to 92.5 mM raised [Mg2+]i in control cells (1.56 ± 0.19 mM) at 30 min, while this effect was significantly attenuated in TRPM7-silenced cells (1.12 ± 0.07 mM). The Mg2+ efflux driven by Na+ gradient was unaffected by TRPM7 silencing. These results suggest that TRPM7 regulates the rate of Mg2+ influx in H9c2 cells, although cytoplasmic Mg2+ homeostasis at basal conditions is unaffected by TRPM7 silencing.
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