Water permeability of aquaporin-4 is decreased by protein kinase C and dopamine

Zelenina, Marina; Zelenin, Sergey; Bondar, Alexander A.; Brismar, Hjalmar; Aperia, Anita

doi:10.1152/ajprenal.00260.2001

Cited by 180 publications

(139 citation statements)

References 66 publications

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“…Numerous MIP proteins are subject to phosphorylation, and the effects on activity are varied, ranging from the stimulation (e.g., the plant MIPs ␣ TIP [Maurel et al, 1995] and PM28A [Johansson et al, 1998]) to the inhibition of water transport (e.g., mammalian AQP4 [Han et al, 1998;Zelenina et al, 2002]) and alterations in water permeability by affecting membrane trafficking and subcellular localization (e.g., AQP4 [Madrid et al, 2001] and AQP2 [Nielsen et al, 1995;Fushimi et al, 1997]). The present study shows that phosphorylation of nodulin 26 enhances its water permeability both upon expression in Xenopus oocytes and in symbiosome membrane vesicles.…”

Section: Discussionmentioning

confidence: 99%

Phosphorylation of Soybean Nodulin 26 on Serine 262 Enhances Water Permeability and Is Regulated Developmentally and by Osmotic Signals

et al. 2003

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Soybean nodulin 26 is expressed and targeted to the symbiosome membrane of nitrogen-fixing nodules, where it forms an aquaporin channel with a modest water transport rate. In this study, we show that the phosphorylation of nodulin 26 on Ser-262, which is catalyzed by a symbiosome membrane-associated calcium-dependent protein kinase, stimulates its intrinsic water transport rate. Furthermore, using a phosphospecific antibody, we have elucidated the developmental appearance and regulation of nodulin 26 phosphorylation in vivo. Although nodulin 26 protein is detected first in differentiating infected cells (16 days), phosphorylated nodulin 26 does not become pronounced until infected cell maturation (25 days). Phosphorylation is sustained at steady state levels until entry into senescence. Nodulin 26 phosphorylation is enhanced further by osmotic stresses (water deprivation and salinity). Thus, the phosphorylation of nodulin 26 coincides with the establishment of mature nitrogen-fixing symbiosomes, is regulated by osmotic stresses that induce calcium-signaling pathways, and appears to be part of the adaptive responses of infected cells to osmotic challenge.

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Section: Discussionmentioning

confidence: 99%

Phosphorylation of Soybean Nodulin 26 on Serine 262 Enhances Water Permeability and Is Regulated Developmentally and by Osmotic Signals

et al. 2003

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“…Decreased glucosuria may be linked to decreased washout of glucose by the concomitant decreased diuresis and effects on renal glucose transporters. Decreased diuresis may be linked to reversal of diabetes-induced activation of protein kinase C by highdose thiamine and benfotiamine [6] and consequent reversal of the inhibition of water re-uptake by aquaporins in renal collecting duct cells [21,22]. In any event, STZ diabetic rats with high-dose thiamine therapy consumed less food than control STZ diabetic rats whilst maintaining similar body weights.…”

Section: Discussionmentioning

confidence: 99%

High-dose thiamine therapy counters dyslipidaemia in streptozotocin-induced diabetic rats

et al. 2004

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Aims/hypothesis. Cardiovascular disease in diabetes is linked to increased risk of atherosclerosis, increased levels of triglyceride-rich lipoproteins and enhanced hepatic lipogenesis. The hepatic hexosamine pathway has been implicated in signalling for de novo lipogenesis by the liver. In this study, we assessed if decrease of flux through the hexosamine pathway induced by high-dose thiamine therapy counters diabetic dyslipidaemia. Methods. The model of diabetes used was the streptozotocin-induced diabetic rat with maintenance insulin therapy. Normal control and diabetic rats were studied for 24 weeks with and without oral high-dose therapy (7 and 70 mg/kg) with thiamine and benfotiamine. Plasma total cholesterol, HDL cholesterol and triglycerides were determined at 6-week intervals and hepatic metabolites and transketolase activity after death of the rats at 24 weeks.Results. We found that thiamine therapy (70 mg/kg) prevented diabetes-induced increases in plasma cholesterol and triglycerides in diabetic rats but did not reverse the diabetes-induced decrease of HDL. This was achieved by prevention of thiamine depletion and decreased transketolase activity in the liver of diabetic rats. There was a concomitant decrease in hepatic UDP-N-acetylglucosamine and fatty acid synthase activity. Thiamine also normalised food intake of diabetic rats. A lower dose of thiamine (7 mg/kg) and the thiamine monophosphate prodrug benfotiamine (7 and 70 mg/kg) were ineffective. Conclusions/interpretation. High-dose thiamine therapy prevented diabetic dyslipidaemia in experimental diabetes probably by suppression of food intake and hexosamine pathway signalling but other factors may also be involved. Benfotiamine was ineffective.Keywords Cholesterol · Dyslipidaemia · Glycation · Hexosamine · Streptozotocin · Thiamine · Triglycerides Abbreviations: 1,3-bis-PG, 1,3-bisphosphoglycerate · ACC, acetyl-CoA carboxylase · CEL, N ε -(1-carboxyethyl)lysine · CML, N ε -carboxymethyl-lysine · CTEP, cholesteryl ester transfer protein · DAG, diacylglycerol · DHAP, dihydroxyacetonephosphate · F-1,6-bis-P, fructose-1,6-bis-phosphate · FAS, fatty acid synthase · FL, N ε -fructosyl-

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“…We used constructs encoding mouse AQP4.M23 tagged with green fluorescent protein (GFP) at the NH2 terminus (pGFP-AQP4.M23), described previously (35,36).…”

Section: Methodsmentioning

confidence: 99%

“…Water permeability (Pf) was measured using a method that we described in detail previously (35,37). By use of this method Pf in individual cells within cell monolayers can be determined and compared between cells that do or do not express GFP-labeled proteins.…”

Section: Methodsmentioning

confidence: 99%

Erythropoietin modulation of astrocyte water permeability as a component of neuroprotection

Gunnarson

Song

Kowalewski

et al. 2009

Proc. Natl. Acad. Sci. U.S.A.

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Disturbed brain water homeostasis with swelling of astroglial cells is a common complication in stroke, trauma, and meningitis and is considered to be a major cause of permanent brain damage. Astroglial cells possess the water channel aquaporin 4 (AQP4). Recent studies from our laboratory have shown that glutamate, acting on group I metabotropic glutamate receptors (mGluRs), increases the permeability of astrocyte AQP4, which, in situations of hypoxia-ischemia, will increase astrocyte water uptake. Here we report that erythropoietin (EPO), which in recent years has emerged as a potent neuro-protective agent, antagonizes the effect of a group I mGluR agonist on astrocyte water permeability. Activation of group I mGluRs triggers fast and highly regular intracellular calcium oscillations and we show that EPO interferes with this signaling event by altering the frequency of the oscillations. These effects of EPO are immediate, in contrast to the neuroprotective effects of EPO that are known to depend upon gene activation. Our findings indicate that EPO may directly reduce the risk of astrocyte swelling in stroke and other brain insults. In support of this conclusion we found that EPO reduced the neurological symptoms in a mouse model of primary brain edema known to depend upon AQP4 water transport.aquaporin 4 ͉ brain edema ͉ glutamate E rythropoietin, the major haemopoietic growth factor, has in recent years emerged as one of the most efficient neuroprotective agents (1-3). It is well documented from both experimental and clinical studies that erythropoietin (EPO) attenuates the degree of brain damage after stroke (4-6). Stroke is associated with a massive release of glutamate and experimental studies have indicated that EPO also protects from glutamatetriggered neurotoxicity (7). EPO acts by preventing the destruction of viable tissue surrounding the site of an injury, that is, the penumbra that develops during the first 24-48 h after a brain insult (1). Cell swelling is one of the characteristic features of the penumbra (8, 9).Mounting evidence suggests that water uptake in astrocytes via the water channel aquaporin 4 (AQP4) is an important factor contributing to post-ischemic cell swelling (10, 11). Immunohistochemical studies have indicated a colocalization between EPO receptors and AQP4 in the brain (12, 13), particularly in glial cells at the interface between the brain parenchyma and the periphery. This raises the question whether EPO may modulate astrocyte water permeability and whether this effect may attenuate astrocyte water uptake after a brain insult. We have in a recent study demonstrated that glutamate increases astrocyte water permeability via activation of AQP4 (14). In the present study we have tested the possibility that EPO may counteract the effect of glutamate on astrocyte water permeability.To document the tissue protective role of EPO in brain edema, we first tested whether EPO reduces symptoms in a mouse model of water intoxication known to depend upon glial AQP4 (11). Observing a robust eff...

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Water permeability of aquaporin-4 is decreased by protein kinase C and dopamine

Cited by 180 publications

References 66 publications

Phosphorylation of Soybean Nodulin 26 on Serine 262 Enhances Water Permeability and Is Regulated Developmentally and by Osmotic Signals

Phosphorylation of Soybean Nodulin 26 on Serine 262 Enhances Water Permeability and Is Regulated Developmentally and by Osmotic Signals

High-dose thiamine therapy counters dyslipidaemia in streptozotocin-induced diabetic rats

Erythropoietin modulation of astrocyte water permeability as a component of neuroprotection

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