The SWELL1-LRRC8 complex regulates endothelial AKT-eNOS signaling and vascular function

Alghanem, Ahmad F.; Abello, Javier; Maurer, Joshua A.; Kumar, Ashutosh; Ta, Chau My; Gunasekar, Susheel K.; Fatima, Urooj; Chen, Kang; Xie, Litao; Adeola, Oluwaseun; Riker, Megan; Elliot-Hudson, Macaulay; Minerath, Rachel A; Grueter, Chad E.; Mullins, Robert F.; Stratman, Amber N.; Sah, Rajan

doi:10.7554/elife.61313

Cited by 43 publications

(52 citation statements)

References 99 publications

(170 reference statements)

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“…In this study (Figure 6), AKT, iNS, eNOS, and MAPK were downregulated in the model group compared with the control group and significantly upregulated in the GP and MET groups compared with the model group. These results were in line with the data presented in previous reports (Alghanem et al, 2021;Cheng et al, 2021). As reported, the AGE-RAGE signaling pathway is closely associated with T2DM and inflammation (Syed et al, 2020).…”

Section: Regulation Of Pi3k/akt and Age-rage Signaling In Vivosupporting

confidence: 93%

Based on Plasma Metabonomics and Network Pharmacology Exploring the Therapeutic Mechanism of Gynura procumbens on Type 2 Diabetes

Guo

Ouyang²,

Liu

et al. 2021

Front. Pharmacol.

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Gynura procumbens (GP) is a perennial herbal medicine and food homologous plant, which has been reported to have a good hypoglycemic effect. However, its active components and underlying mechanism of action are not clear. Here, we aimed to confirm the effects of GP on type 2 diabetes (T2DM) from several different aspects. We used UPLC/Q-TOF MS to analyze the metabolic patterns, which included blood samples of clinical subjects and db/db mice to screen for serum metabolic markers and metabolic pathways. We also used network pharmacology to study GP targets in the treatment of T2DM. Data from endogenous metabolites in plasma showed that two common pathways, including glycerol phosphate metabolism and retinol metabolism, were identified in plasma samples of the groups. Finally, Western blot analysis was used to verify the expression of proteins in the PI3K/AKT and AGE–RAGE signaling pathways. The protein expression of AKT, eNOS, iNS, and MAPK was significantly upregulated, and the expression of caspase-8 and caspase-3 was significantly downregulated. Thus, our findings indicated that GP could alleviate insulin resistance by regulating biometabolic markers and key proteins in the PI3K/AKT and AGE–RAGE signaling pathways to treat T2DM.

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Section: Regulation Of Pi3k/akt and Age-rage Signaling In Vivosupporting

confidence: 93%

Based on Plasma Metabonomics and Network Pharmacology Exploring the Therapeutic Mechanism of Gynura procumbens on Type 2 Diabetes

Guo

Ouyang²,

Liu

et al. 2021

Front. Pharmacol.

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“…The identification of the LRRC8 gene family has revitalized the VRAC field, by confirming previously suspected roles and discovering new roles in adipocyte physiology, insulin signaling, vascular physiology, sperm development, drug uptake, immune responses to virus infection, and neurotransmitter release in the brain (22)(23)(24)(25)(26)(27)(28)(29)(30)(31). Many of these studies have highlighted the need for developing potent and specific pharmacological tools for probing the physiology and therapeutic potential of VRAC in human diseases.…”

Section: Introductionmentioning

confidence: 99%

Zinc pyrithione activates the volume-regulated anion channel through an antioxidant-sensitive mechanism

Figueroa

Denton

2021

American Journal of Physiology-Cell Physiology

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LRRC8 volume-regulated anion channels (VRACs) play important roles in diverse cell types and may represent therapeutic targets for diseases. To date, however, the pharmacological tools for evaluating the druggability of VRAC have been limited to inhibitors, as no activators of the channel have been reported. We performed a fluorescence-based high-throughput screen (HTS) of 1,184 FDA-approved drugs for compounds that increase VRAC activity. The most potent VRAC potentiator identified was zinc pyrithione (ZPT), which is used commercially for treating dandruff and other skin disorders. In intracellular YFP(F46L/H148Q/I152L)-quenching assays, ZPT potentiates the rate and extent of swelling-induced iodide influx dose-dependently with a half-maximal effective concentration (EC50) of 5.7 µM. Whole-cell voltage-clamp experiments revealed that co-application of hypotonic solution and 30 µM ZPT to HEK293 or HCT116 cells increases the rate of swelling-induced VRAC activation by approximately 10-fold. ZPT potentiates swelling-induced VRAC currents after currents have reached a steady state and activates currents in the absence of cell swelling. Neither ZnCl2 nor free pyrithione activated VRAC, however, treating cells with a mixture of ZnCl2 and pyrithione led to robust channel activation. Finally, the effects of ZPT on VRAC were inhibited by reactive oxygen species (ROS) scavenger NAC and NAD(P)H oxidase inhibitor DPI, suggesting the mechanism of action involves ROS generation. The discovery of ZPT as a potentiator/activator of VRAC demonstrates the utility of HTS for identifying small-molecule modulators of VRAC and adds to a growing repertoire of pharmacological tool compounds for probing the molecular physiology and regulation of this important channel.

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“…Hypotonic swelling has been shown to promote the release of NO and reactive nitrogen oxide species in various cells ( Kimura et al, 2000 ; Haussinger and Schliess, 2005 ; Takeda-Nakazawa et al, 2007 ; Kruczek et al, 2009 ; Gonano et al, 2014 ) and to augment LPS-triggered iNOS expression in RAW 264.7 macrophages ( Warskulat et al, 1998 ). Recently, it has been shown that in HUVECs, VRAC/SWELL1/LRRC8A mediates endothelial cell alignment via stretch-dependent Akt-eNOS signaling and formation of a signaling complex made up by Grb2, Cav-1, and eNOS ( Alghanem et al, 2021 ).…”

Section: Water Ions and Their Channels And Transporters In Pinocytosismentioning

confidence: 99%

“…LRRC8A-E/SWELL1 proteins are essential components of the volume-regulated outwardly rectifying Cl – current (VRAC, VSOR, VSOAC, ICl swell , ICl vol ) elicited in most cells during cell swelling ( Qiu et al, 2014 ; Voss et al, 2014 ; Jentsch, 2016 ; Jentsch et al, 2016 ; Okada, 2020 ; Bertelli et al, 2021 ), and they are involved in a broad variety of cellular functions ( Chen et al, 2019 ). LRRC8A-E/SWELL1 also regulate the PI3K-Akt, Erk1/2, mTOR signaling cascade ( Kumar et al, 2020 ; Alghanem et al, 2021 ). Recently, Li et al (2020) demonstrated the expression of LRRC8 family members on lysosomal membranes and their ability to build functional lysosomal VRACs (Lyso-VRACs).…”

Section: Water Ions and Their Channels And Transporters In Pinocytosismentioning

confidence: 99%

From Pinocytosis to Methuosis—Fluid Consumption as a Risk Factor for Cell Death

Ritter

Bresgen

Kerschbaum

2021

Front. Cell Dev. Biol.

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The volumes of a cell [cell volume (CV)] and its organelles are adjusted by osmoregulatory processes. During pinocytosis, extracellular fluid volume equivalent to its CV is incorporated within an hour and membrane area equivalent to the cell’s surface within 30 min. Since neither fluid uptake nor membrane consumption leads to swelling or shrinkage, cells must be equipped with potent volume regulatory mechanisms. Normally, cells respond to outwardly or inwardly directed osmotic gradients by a volume decrease and increase, respectively, i.e., they shrink or swell but then try to recover their CV. However, when a cell death (CD) pathway is triggered, CV persistently decreases in isotonic conditions in apoptosis and it increases in necrosis. One type of CD associated with cell swelling is due to a dysfunctional pinocytosis. Methuosis, a non-apoptotic CD phenotype, occurs when cells accumulate too much fluid by macropinocytosis. In contrast to functional pinocytosis, in methuosis, macropinosomes neither recycle nor fuse with lysosomes but with each other to form giant vacuoles, which finally cause rupture of the plasma membrane (PM). Understanding methuosis longs for the understanding of the ionic mechanisms of cell volume regulation (CVR) and vesicular volume regulation (VVR). In nascent macropinosomes, ion channels and transporters are derived from the PM. Along trafficking from the PM to the perinuclear area, the equipment of channels and transporters of the vesicle membrane changes by retrieval, addition, and recycling from and back to the PM, causing profound changes in vesicular ion concentrations, acidification, and—most importantly—shrinkage of the macropinosome, which is indispensable for its proper targeting and cargo processing. In this review, we discuss ion and water transport mechanisms with respect to CVR and VVR and with special emphasis on pinocytosis and methuosis. We describe various aspects of the complex mutual interplay between extracellular and intracellular ions and ion gradients, the PM and vesicular membrane, phosphoinositides, monomeric G proteins and their targets, as well as the submembranous cytoskeleton. Our aim is to highlight important cellular mechanisms, components, and processes that may lead to methuotic CD upon their derangement.

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The SWELL1-LRRC8 complex regulates endothelial AKT-eNOS signaling and vascular function

Cited by 43 publications

References 99 publications

Based on Plasma Metabonomics and Network Pharmacology Exploring the Therapeutic Mechanism of Gynura procumbens on Type 2 Diabetes

Based on Plasma Metabonomics and Network Pharmacology Exploring the Therapeutic Mechanism of Gynura procumbens on Type 2 Diabetes

Zinc pyrithione activates the volume-regulated anion channel through an antioxidant-sensitive mechanism

From Pinocytosis to Methuosis—Fluid Consumption as a Risk Factor for Cell Death

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