| Literature DB >> 27956381 |
Ming-Ming Wu1,2, Yu-Jia Zhai2, Yu-Xia Li1, Qing-Qing Hu1, Zhi-Rui Wang1, Shi-Peng Wei2, Li Zou2, Abdel A Alli2, Tiffany L Thai2, Zhi-Ren Zhang3, He-Ping Ma2.
Abstract
A Ca2+-activated nonselective cation channel (NSCCa) is found in principal cells of the mouse cortical collecting duct (CCD). However, the molecular identity of this channel remains unclear. We used mpkCCDc14 cells, a mouse CCD principal cell line, to determine whether NSCCa represents the transient receptor potential (TRP) channel, the melastatin subfamily 4 (TRPM4). A Ca2+-sensitive single-channel current was observed in inside-out patches excised from the apical membrane of mpkCCDc14 cells. Like TRPM4 channels found in other cell types, this channel has an equal permeability for Na+ and K+ and has a linear current-voltage relationship with a slope conductance of ~23 pS. The channel was inhibited by a specific TRPM4 inhibitor, 9-phenanthrol. Moreover, the frequency of observing this channel was dramatically decreased in TRPM4 knockdown mpkCCDc14 cells. Unlike those previously reported in other cell types, the TRPM4 in mpkCCDc14 cells was unable to be activated by hydrogen peroxide (H2O2). Conversely, after treatment with H2O2, TRPM4 density in the apical membrane of mpkCCDc14 cells was significantly decreased. The channel in intact cell-attached patches was activated by ionomycin (a Ca2+ ionophore), but not by ATP (a purinergic P2 receptor agonist). These data suggest that the NSCCa current previously described in CCD principal cells is actually carried through TRPM4 channels. However, the physiological role of this channel in the CCD remains to be further determined.Entities:
Keywords: Ca2+-activated nonselective cation channel; confocal microscopy; intracellular calcium; patch clamp; reactive oxygen species
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Year: 2016 PMID: 27956381 PMCID: PMC5210207 DOI: 10.1152/ajprenal.00439.2016
Source DB: PubMed Journal: Am J Physiol Renal Physiol ISSN: 1522-1466