Pannexin 1 channels in renin-expressing cells influence renin secretion and blood pressure homeostasis

DeLalio, Leon J.; Masati, Ester; Mendu, Suresh K.; Ruddiman, Claire A.; Yang, Yang; Johnstone, Scott R.; Milstein, Jenna; Keller, Thomas C. S.; Weaver, Rachel B.; Guagliardo, Nick A.; Best, Angela K.; Ravichandran, Kodi S.; Bayliss, Douglas A.; Sequeira-Lόpez, Maria Luisa S.; Sonkusare, Swapnil N.; Shu, Xiaohong; Desai, Bimal N.; Barrett, Paula Q.; Le, Thu H.; Gomez, R. Ariel; Isakson, Brant E.

doi:10.1016/j.kint.2020.04.041

Cited by 17 publications

(20 citation statements)

References 79 publications

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“…Moreover, not only cell–cell communication via gap junctions seems to be important for the regulation of renin secretion but also signaling via connexin hemichannels [ 36 ]. A recent study suggests that pannexin 1 could also be involved in the regulation of basal renin secretion through mediating intercellular communication [ 14 ]. Another cell adhesion molecule essential for mediating cell–cell or cell–matrix interactions is β1-integrin, which is abundantly expressed in the kidneys including renin-lineage cells.…”

Section: Identity Of Renin-expressing Cellsmentioning

confidence: 99%

Flexible and multifaceted: the plasticity of renin-expressing cells

Broeker

Schrankl

Fuchs

et al. 2022

Pflugers Arch - Eur J Physiol

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The protease renin, the key enzyme of the renin–angiotensin–aldosterone system, is mainly produced and secreted by juxtaglomerular cells in the kidney, which are located in the walls of the afferent arterioles at their entrance into the glomeruli. When the body’s demand for renin rises, the renin production capacity of the kidneys commonly increases by induction of renin expression in vascular smooth muscle cells and in extraglomerular mesangial cells. These cells undergo a reversible metaplastic cellular transformation in order to produce renin. Juxtaglomerular cells of the renin lineage have also been described to migrate into the glomerulus and differentiate into podocytes, epithelial cells or mesangial cells to restore damaged cells in states of glomerular disease. More recently, it could be shown that renin cells can also undergo an endocrine and metaplastic switch to erythropoietin-producing cells. This review aims to describe the high degree of plasticity of renin-producing cells of the kidneys and to analyze the underlying mechanisms.

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Section: Identity Of Renin-expressing Cellsmentioning

confidence: 99%

Flexible and multifaceted: the plasticity of renin-expressing cells

Broeker

Schrankl

Fuchs

et al. 2022

Pflugers Arch - Eur J Physiol

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“…As a control to rule out ATP secretion by connexins, we found that the Cx43 peptide inhibitor Gap19 did not affect EFS-induced constriction (Figure 4D-F and Supplemental Figure 6). Genetic Panx1 deletion has been used to demonstrate an important role in blood pressure regulation by renin-secreting cells 18 (where genetic deletion causes hypertension) and by SMC 3 (where genetic deletion causes hypotension). Because iSMC Panx1 OE mice displayed increased EFS induced vasoconstriction we hypothesized these mice would have elevated blood pressure.…”

Section: Resultsmentioning

confidence: 99%

Amount of Pannexin 1 in smooth muscle cells regulates sympathetic nerve induced vasoconstriction

Dunaway

Billaud

Macal

et al. 2022

Preprint

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Pannexin 1 (Panx1) forms high conductance channels that secrete ATP upon stimulation. The role of Panx1 in mediating constriction in response to direct sympathetic nerve stimulation is not known. Additionally, it is unknown how the expression level of Panx1 in SMCs influences a-adrenergic responses. We hypothesized that the amount of Panx1 in SMCs dictates the levels of sympathetic constriction and blood pressure. To test this hypothesis, we used genetically modified mouse models enabling expression of Panx1 in vascular cells to be varied. Genetic deletion of SMC Panx1 prevented constriction by electric field stimulation of sympathetic nerves. Conversely, over-expression of Panx1 in SMCs using a ROSA26 transgenic model increased sympathetic nerve-mediated constriction. Cx43 hemichannel inhibitors did not alter constriction. Next, we evaluated the effects of altered SMC Panx1 expression on blood pressure. To do this, we created mice combining a global Panx1 deletion, with ROSA26-Panx1 under the control of an inducible SMC specific Cre (Myh11). This resulted in mice that could express only human Panx1, only in SMCs. After tamoxifen, these mice had increased blood pressure that was acutely decreased by the Panx1 inhibitor spironolactone. Control mice genetically devoid of Panx1 did not respond to spironolactone. These data suggest Panx1 in SMCs could regulate the extent of sympathetic nerve constriction and blood pressure. The results also show the feasibility humanized Panx1-mouse models to test pharmacological candidates.

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“…The vast majority of work has focused on Panx1 as an ATP channel, with multiple stimuli inducing ATP secretion as a paracrine signaling pathway. However, physiologic roles for Panx1 are not limited to secretion, as more recent evidence has shown that Panx1 can also act as a plasma membrane calcium channel, increasing cytosolic calcium in response to stimuli, such as TNFα [ 29 , 30 ]. Several other solutes have been shown to be transmitted through Panx1 including fluorescent tracers, anandamide, lactate, glutamate, spermidine, and bacterial products, consistent with roles for Panx1 in multiple different signaling pathways [ 26 , 27 , 31 – 33 ].…”

Section: Pannexin 1 Structure Function and Post-translational Modificationsmentioning

confidence: 99%

“…This is in comparison to constitutive phosphorylation of Y198 on the intracellular loop of Panx1 which was found to be important for Panx1 channel opening. A mimetic peptide against this region (“PxIL2P”) was able to inhibit Panx1 current, ATP release, and alpha-adrenergic vasoconstriction; more general Panx1 inhibition was also noted in endothelium and renin-secreting cells [ 5 – 7 , 30 , 49 , 59 ]. Although the Y308 site has not been found to be as important in terms of plasma membrane localization or trafficking, it is similar to Y198, in that it was important for gating properties, including ATP release and current [ 10 , 60 ].…”

Section: Pannexin 1 Structure Function and Post-translational Modificationsmentioning

confidence: 99%

“…Panx1 is present throughout the kidney, especially in the vasculature, apical membranes of proximal tubules, collecting ducts, and thick descending limbs [ 100 ]. Regulation of ATP levels by Panx1 mediated release in the kidney is essential under physiological conditions, since it regulates renal hemodynamics and tubular transport in addition to pathological conditions [ 101 ]. Pharmacological and genetic screening methods of assessing the effects of Panx1 on renal IRI [ 14 ], a mouse model of AKI, revealed that global, endothelial, and epithelial tissue-specific deletion of Panx1 had a protective effect, as did pharmacological inhibition of Panx1 channels during AKI [ 14 , 102 ].…”

Section: Kidneymentioning

confidence: 99%

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Pannexin 1 as a driver of inflammation and ischemia–reperfusion injury

Koval

Cwiek

Carr

et al. 2021

Purinergic Signalling

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Pannexin 1 (Panx1) is a ubiquitously expressed protein forming large conductance channels that are central to many distinct inflammation and injury responses. There is accumulating evidence showing ATP released from Panx1 channels, as well as metabolites, provide effective paracrine and autocrine signaling molecules that regulate different elements of the injury response. As channels with a broad range of permselectivity, Panx1 channels mediate the secretion and uptake of multiple solutes, ranging from calcium to bacterial derived molecules. In this review, we describe how Panx1 functions in response to different pro-inflammatory stimuli, focusing mainly on signaling coordinated by the vasculature. How Panx1 mediates ATP release by injured cells is also discussed. The ability of Panx1 to serve as a central component of many diverse physiologic responses has proven to be critically dependent on the context of expression, post-translational modification, interacting partners, and the mode of stimulation.

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Pannexin 1 channels in renin-expressing cells influence renin secretion and blood pressure homeostasis

Cited by 17 publications

References 79 publications

Flexible and multifaceted: the plasticity of renin-expressing cells

Flexible and multifaceted: the plasticity of renin-expressing cells

Amount of Pannexin 1 in smooth muscle cells regulates sympathetic nerve induced vasoconstriction

Pannexin 1 as a driver of inflammation and ischemia–reperfusion injury

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