Polycystin-2 is an essential ion channel subunit in the primary cilium of the renal collecting duct epithelium

Liu, Xiaowen; Vien, Thuy N.; Duan, Jingjing; Sheu, Shu-Hsien; DeCaen, Paul G.; Clapham, David E.

doi:10.7554/elife.33183

Cited by 139 publications

(197 citation statements)

References 86 publications

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“…Thirdly, our results show that the PC1/PC2_AA channel has a larger or more flexible pore, and higher permeability to most monovalent cations tested in this study (i.e., Na + , Li + , Cs + , DMA + , DEA + , and TEA + ) when compared to PC2_AA alone (Fig 5). The fact that the homomeric PC2 channel has low Ca 2+ permeability [11,22] while the PC1/PC2 channel complex has much higher Ca 2+ permeability indicates their very distinct physiological roles and thus contributions to ADPKD. Collectively, these results tell us that the heteromeric PC1/PC2 channel and the homomeric PC2 channel are two distinct channels that likely have their unique functions.…”

Section: Discussionmentioning

confidence: 99%

“…How these mutations lead to ADPKD is unclear, and the molecular mechanism of the function of the PC1/PC2 complex is largely unknown. The Ca 2+ conductance by PC2 or PC1/PC2 complex is also hotly debated [7,[9][10][11][12][13][14][15][16]. However, thus far the in vivo stimuli of this complex remain unknown, although previous studies suggested fluid flow as the potential stimulus [8] and Wnt proteins as candidate ligands [9].…”

Section: Introductionmentioning

confidence: 99%

“…This complex shares overall structural similarity to the homotetrameric PC2 channel, with the last two transmembrane domains (S10-S11) of PC1 directly participating in forming the presumed channel pore [42]. PC2_F640P gave rise to robust whole-oocyte currents when expressed in Xenopus laevis oocytes [11,22,43]. This is mainly due to the lack of knowledge on the channel activation mechanism, making functional analysis very challenging.…”

Section: Introductionmentioning

confidence: 99%

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The ion channel function of polycystin‐1 in the polycystin‐1/polycystin‐2 complex

Wang

Liu

et al. 2019

EMBO Reports

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Autosomal dominant polycystic kidney disease (ADPKD) is caused by mutations in PKD1 or PKD2 gene, encoding the polycystic kidney disease protein polycystin‐1 and the transient receptor potential channel polycystin‐2 (also known as TRPP2), respectively. Polycystin‐1 and polycystin‐2 form a receptor–ion channel complex located in primary cilia. The function of this complex, especially the role of polycystin‐1, is largely unknown due to the lack of a reliable functional assay. In this study, we dissect the role of polycystin‐1 by directly recording currents mediated by a gain‐of‐function (GOF) polycystin‐1/polycystin‐2 channel. Our data show that this channel has distinct properties from that of the homomeric polycystin‐2 channel. The polycystin‐1 subunit directly contributes to the channel pore, and its eleven transmembrane domains are sufficient for its channel function. We also show that the cleavage of polycystin‐1 at the N‐terminal G protein‐coupled receptor proteolysis site is not required for the activity of the GOF polycystin‐1/polycystin‐2 channel. These results demonstrate the ion channel function of polycystin‐1 in the polycystin‐1/polycystin‐2 complex, enriching our understanding of this channel and its role in ADPKD.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The ion channel function of polycystin‐1 in the polycystin‐1/polycystin‐2 complex

Wang

Liu

et al. 2019

EMBO Reports

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“…renal cortical collecting duct cells [139,140], where they were initially proposed to form a receptor-channel complex [141] that functions as a mechanosensitive Ca 2+ channel activated by fluid flow [142]. This hypothesis has been challenged by others [143,144], and recent work from David Clapham's lab using primary cultures of collecting duct cells isolated from kidneys of a new ADPKD mouse model, indicated that PC2, but not PC1, constitutes an essential ion channel subunit in the primary cilium that preferentially conducts K + and Na + and is potentiated by intraciliary Ca 2+ [145]. This study also showed that ciliary trafficking of PC2 occurs independently of PC1, contradicting several earlier reports [16,145], but in agreement with the recently solved homotetrameric structure of PC2 [146,147].…”

Section: Polycystin Signallingmentioning

confidence: 99%

Regulation of ciliary membrane protein trafficking and signalling by kinesin motor proteins

2018

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Primary cilia are antenna-like sensory organelles that regulate a substantial number of cellular signalling pathways in vertebrates, both during embryonic development as well as in adulthood, and mutations in genes coding for ciliary proteins are causative of an expanding group of pleiotropic diseases known as ciliopathies. Cilia consist of a microtubule-based axoneme core, which is subtended by a basal body and covered by a bilayer lipid membrane of unique protein and lipid composition. Cilia are dynamic organelles, and the ability of cells to regulate ciliary protein and lipid content in response to specific cellular and environmental cues is crucial for balancing ciliary signalling output. Here we discuss mechanisms involved in regulation of ciliary membrane protein trafficking and signalling, with main focus on kinesin-2 and kinesin-3 family members.

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“…Mutations in the pkd1 and pdk2 genes are associated with ADPKD. These genes encode the polycystins, PC1 & 2, the latter, referred to as TRPP2 (transient receptor potential polycystic), functions as a non-selective cation channel[3] [4]. Malfunction of either PC1 or PC2 leads to cyst formation [5]…”

Section: Introductionmentioning

confidence: 99%

Role of calcium in adult onset polycystic kidney disease

Yanda

Liu

Cebotaru

et al. 2019

Cellular Signalling

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Autosomal dominant polycystic kidney disease (ADPKD) is caused by mutations in genes encoding the polycystin (PC) 1 and 2 proteins. The goal of this study was to determine the role of calcium in regulating cyst growth. Stromal interaction molecule 1 (STIM1) protein expression was 15-fold higher in PC1-null proximal tubule cells (PN) than in heterozygote (PH) controls and 2-fold higher in an inducible, PC1 knockout, mouse model of ADPKD compared to a non-cystic match control. IP3 receptor protein expression was also higher in the cystic mice. Knocking down STIM1 with siRNA reduced cyst growth and lowered cAMP levels in PN cells. Fura2 measurements of intracellular Ca2+ showed a dramatic reduction in thapsigargin-stimulated release of ER Ca2+ following STIM1 silencing or application of 2-APB, consistent with altered ER Ca2+ movement; the protein expression of the Ca2+-dependent adenylyl cyclases (AC) AC3 and AC6 was up- and down-regulated, respectively. Like STIM1 knockdown, application of the calmodulin inhibitor W7 lowered cAMP levels, further indicating that STIM1 regulates AC3 via Ca2+ We conclude that the high levels of STIM1 in ADPKD cells play a role in supporting cyst growth and promoting high cAMP levels and an increased release of Ca2+ from the ER. Thus, our results provide novel therapeutic targets for treating ADPKD.

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Polycystin-2 is an essential ion channel subunit in the primary cilium of the renal collecting duct epithelium

Cited by 139 publications

References 86 publications

The ion channel function of polycystin‐1 in the polycystin‐1/polycystin‐2 complex

The ion channel function of polycystin‐1 in the polycystin‐1/polycystin‐2 complex

Regulation of ciliary membrane protein trafficking and signalling by kinesin motor proteins

Role of calcium in adult onset polycystic kidney disease

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