Exocytotic Insertion of TRPC6 Channel into the Plasma Membrane upon Gq Protein-coupled Receptor Activation

Cayouette, Sylvie; Lussier, Marc; Mathieu, Eve-Lyne; Bousquet, Simon M.; Boulay, Guylain

doi:10.1074/jbc.m312042200

Cited by 172 publications

(138 citation statements)

References 61 publications

(64 reference statements)

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“…We also examined TRPC6 because a microarray analysis suggested that it was up-regulated in T1R3 knockdown cells. Carbachol is capable of inducing ROCE by activating and promoting cell surface expression of TRPC6 downstream of muscarinic receptor binding (26,27). Although the suspected change in its mRNA could not be validated, TRPC6 seemed a logical candidate and may be involved in some manner we did not detect (23,24).…”

Section: Discussioncontrasting

confidence: 45%

“…Calcium entry occurring through plasma membrane channels as a result of GPCR activation independent of the state of Ca 2ϩ i stores is referred to as ROCE (25). It has been demonstrated that carbachol is capable of inducing ROCE by activating and promoting cell surface expression of TRPC6 downstream of muscarinic receptor binding (26,27). Expression of neither RGS4 nor TRPC6 was significantly different in T1R3 knockdown cells compared with the control, suggesting that the enhanced carbachol response was not a result of decreased RGS4 or increased TRPC6 expression (Fig.…”

Section: Carbachol-induced Changes In Camentioning

confidence: 99%

See 1 more Smart Citation

Muscarinic Control of MIN6 Pancreatic β Cells Is Enhanced by Impaired Amino Acid Signaling

Guerra¹,

Wauson

McGlynn

et al. 2014

Journal of Biological Chemistry

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Background: Depletion of the GPCR T1R1/T1R3 increased calcium and ERK1/2 signaling by carbachol. Results: T1R3 depletion or reducing amino acids overnight increased M3 muscarinic receptor expression and altered calcium responses. Conclusion: M3 receptor expression in ␤ cells is up-regulated by reduced amino acid availability. Significance: The M3 muscarinic receptor is a potential therapeutic target in ␤ cells with impaired amino acid sensitivity.

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Section: Discussioncontrasting

confidence: 45%

Section: Carbachol-induced Changes In Camentioning

confidence: 99%

Muscarinic Control of MIN6 Pancreatic β Cells Is Enhanced by Impaired Amino Acid Signaling

Guerra¹,

Wauson

McGlynn

et al. 2014

Journal of Biological Chemistry

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“…The presence of a channel at the cell membrane must be tightly controlled to ensure correct timing and duration of signals relayed by such proteins. Activation of several channels belonging to the TRP family of channels correlates with their increased appearance at the plasma membrane (53)(54)(55). The molecular nature of AA-activated, calcium-permeable channels in the plasma membrane is still unknown.…”

Section: Discussionmentioning

confidence: 99%

Arachidonic Acid–Induced Ca2+ Entry Is Involved in Early Steps of Tumor Angiogenesis

Fiorio

Grange

Antoniotti

et al. 2008

Molecular Cancer Research

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Growth factor -induced intracellular calcium signals in endothelial cells regulate cytosolic and nuclear events involved in the angiogenic process. Among the intracellular messengers released after proangiogenic stimulation, arachidonic acid (AA) plays a key role and its effects are strictly related to calcium homeostasis and cell proliferation. Here, we studied AA-induced intracellular calcium signals in endothelial cells derived from human breast carcinomas (B-TEC). AA promotes B-TEC proliferation and organization of vessel-like structures in vitro. The effect is directly mediated by the fatty acid without a significant contribution of its metabolites. AA induces Ca 2+ i signals in the entire capillary-like structure during the early phases of tubulogenesis in vitro. No such responses are detectable in B-TECs organized in more structured tubules. In B-TECs growing in monolayer, AA induces two different signals: a Ca 2+ i increase due to Ca 2+ entry and an inhibition of store-dependent Ca 2+ entry induced by thapsigargin or ATP. An inhibitor of Ca 2+ entry and angiogenesis, carboxyamidotriazole, significantly and specifically decreases AA-induced B-TEC tubulogenesis, as well as AA-induced Ca 2+ signals in B-TECs. We conclude that (a) AA-activated Ca 2+ entry is associated with the progression through the early phases of angiogenesis, mainly involving proliferation and tubulogenesis, and it is down-regulated during the reorganization of tumor-derived endothelial cells in capillary-like structures; and (b) inhibition of AA-induced Ca 2+ entry may contribute to the antiangiogenic action of carboxyamidotriazole. (Mol Cancer Res 2008;6(4):535 -45)

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“…Another study reported translocation of TRPC3 in response to stimulation of the EGF receptor but failed to observe translocation of TRPC3 in response to M3 receptor stimulation [50]. Stimulation of the M3 receptor causes the translocation of TRPC6 to the plasma membrane [51], and stimulation EGF receptor caused the translocation of TRPC4 [52] and TRPC5 [53] to the plasma membrane. The PI3-kinase pathway and its downstream effector Rac1 are implicated in the EGFstimulated translocation of TRPC5 [53], which may be a general mechanism mediating Tyrosine kinase receptor mediated translocation of TRPC channels.…”

Section: Homer1 and Translocation Of Trpc Channelsmentioning

confidence: 99%

Homer proteins in Ca2+ signaling by excitable and non-excitable cells

et al. 2007

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Homers are scaffolding proteins that bind Ca 2+ signaling proteins in cellular microdomains. The Homers participate in targeting and localization of Ca 2+ signaling proteins in signaling complexes. However, recent work showed that the Homers are not passive scaffolding proteins, but rather they regulate the activity of several proteins within the Ca 2+ signaling complex in an isoform specific manner. Homer2 increases the GAP activity of RGS proteins and PLCβ that accelerate the GTPase activity of Gα subunits. Homer1 gates the activity of TRPC channels, controls the rates of their translocation and retrieval from the plasma membrane and mediates the conformational coupling between TRPC channels and IP 3 Rs. Homer1 stimulates the activity of the cardiac and neuronal Ltype Ca 2+ channels Ca v 1.2 and Ca v 1.3. Homer1 also mediates the communication between the cardiac and smooth muscle ryanodine receptor RyR2 and Ca v 1.2 to regulate E-C coupling. In many cases the Homers function as a buffer to reduce the intensity of Ca 2+ signaling and create a negative bias that can be reversed by the immediate early gene form of Homer 1. Hence, the Homers should be viewed as the buffers of Ca 2+ signaling that ensure a high spatial and temporal fidelity of the Ca 2+ signaling and activation of downstream effects.

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Exocytotic Insertion of TRPC6 Channel into the Plasma Membrane upon Gq Protein-coupled Receptor Activation

Cited by 172 publications

References 61 publications

Muscarinic Control of MIN6 Pancreatic β Cells Is Enhanced by Impaired Amino Acid Signaling

Muscarinic Control of MIN6 Pancreatic β Cells Is Enhanced by Impaired Amino Acid Signaling

Arachidonic Acid–Induced Ca2+ Entry Is Involved in Early Steps of Tumor Angiogenesis

Homer proteins in Ca2+ signaling by excitable and non-excitable cells

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