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KMID : 0811720230270020187
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Korean Journal of Physiology & Pharmacology
2023 Volume.27 No. 2 p.187 ~ p.196
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Negative self-regulation of transient receptor potential canonical 4 by the specific interaction with phospholipase C-¥ä1
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Ko Ju-Yeon
Kim Jin-Hyeong
Myeong Jong-Yun
Kwak Mi-Sun
So In-Suk
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Abstract
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Transient receptor potential canonical (TRPC) channels are non-selective calcium-permeable cation channels. It is suggested that TRPC4¥â is regulated by phospholipase C (PLC) signaling and is especially maintained by phosphatidylinositol 4,5-bisphosphate (PIP2). In this study, we present the regulation mechanism of the TRPC4 channel with PIP2 hydrolysis which is mediated by a channel-bound PLC¥ä1 but not by the GqPCR signaling pathway. Our electrophysiological recordings demonstrate that the Ca2+ via an open TRPC4 channel activates PLC¥ä1 in the physiological range, and it causes the decrease of current amplitude. The existence of PLC¥ä1 accelerated PIP2 depletion when the channel was activated by an agonist. Interestingly, PLC¥ä1 mutants which have lost the ability to regulate PIP2 level failed to reduce the TRPC4 current amplitude. Our results demonstrate that TRPC4 self-regulates its activity by allowing Ca2+ ions into the cell and promoting the PIP2 hydrolyzing activity of PLC¥ä1.
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KEYWORD
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Calcium, Fluorescence resonance energy transfer, Phosphatidylinositols, Phospholipase C delta, Transient receptor potential channels
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