Interactions of Human Organic Anion Transporters with Diuretics

Hasannejad, Habib; Takeda, Michio; Taki, Kentarou; Shin, Ho Jung; Babu, Ellappan; Jutabha, Promsuk; Khamdang, Suparat; Aleboyeh, Mahmoud; Onozato, Maristela L.; Tojo, Akihiro; Enomoto, Atsushi; Anzai, Naohiko; Narikawa, Shinichi; Huang, Xiu-Lin; Niwa, Toshimitsu; Endou, Hitoshi

doi:10.1124/jpet.103.059139

Cited by 184 publications

(131 citation statements)

References 25 publications

(37 reference statements)

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“…Furosemide and bendroflumethiazide inhibited tracer uptake with IC 50 values for mOat1 of 8 Ϯ 1 and 8 Ϯ 3 M, respectively (Fig. 1A), which were comparable with previously reported K i values for rat and human OAT1 (13,36). The IC 50 values for furosemide and bendroflumethiazide in mOat3 were 2.8 Ϯ 0.1 and 21 Ϯ 3 M, respectively (Fig.…”

Section: Resultssupporting

confidence: 79%

“…The IC 50 values for furosemide and bendroflumethiazide in mOat3 were 2.8 Ϯ 0.1 and 21 Ϯ 3 M, respectively (Fig. 1B), also comparable with values previously obtained for human OAT3 in one prior study (13). Thus both furosemide and bendroflumethiazide inhibited tracer uptake by mOat1 and mOat3 in a concentration-dependent manner, consistent with their being substrates for these transporters.…”

Section: Resultssupporting

confidence: 76%

“…Previous expression studies in Xenopus oocytes with rat OAT1 (36) or in mouse S2 cell lines with human OAT1 and human OAT3 (13) had indicated that, in vitro, both OAT1 and OAT3 can transport thiazides as well as loop diuretics, but the in vivo relevance of these transport mechanisms remained unclear. Because of the tremendous clinical importance of diuretic handling by the kidney, it is important to examine transport in vivo.…”

mentioning

confidence: 99%

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Overlapping in vitro and in vivo specificities of the organic anion transporters OAT1 and OAT3 for loop and thiazide diuretics

Vallon¹,

Rieg²,

Ahn³

et al. 2008

American Journal of Physiology-Renal Physiology

116

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Section: Resultssupporting

confidence: 79%

Section: Resultssupporting

confidence: 76%

mentioning

confidence: 99%

See 1 more Smart Citation

Overlapping in vitro and in vivo specificities of the organic anion transporters OAT1 and OAT3 for loop and thiazide diuretics

Vallon¹,

Rieg²,

Ahn³

et al. 2008

American Journal of Physiology-Renal Physiology

116

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“…Organic anion transporter 1 (OAT1/SLC22A6) and OAT3 (SLC22A8) have broad substrate specificities, and kinetic analyses using rat kidney slices have suggested that Oat1 mainly is responsible for the renal uptake of hydrophilic and small organic anions, whereas Oat3 is responsible for the uptake of more bulky organic anions (8 -10). Diuretics interact with OAT1 and OAT3, and, particularly, loop diuretics such as furosemide and bumetanide are substrates of OAT (11,12). Recently, Oat1 knockout mice were generated, and it was demonstrated that Oat1 was responsible for the renal uptake and pharmacologic action of furosemide (13).…”

mentioning

confidence: 99%

Multidrug Resistance–Associated Protein 4 Is Involved in the Urinary Excretion of Hydrochlorothiazide and Furosemide

Hasegawa

Kusuhara

Adachi

et al. 2007

Journal of the American Society of Nephrology

109

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The role of ATP-binding cassette transporters in the urinary excretion of diuretics was investigated. Significant ATPdependent uptake of hydrochlorothiazide (HCT) and furosemide was observed in membrane vesicles that expressed multidrug resistance-associated protein 4 (MRP4) and breast cancer resistance protein (BCRP). Unlike taurocholate uptake, S-methylglutathione had no effect on the ATP-dependent uptake of both compounds by MRP4. The functional importance of MRP4 and BCRP in the urinary excretion of HCT and furosemide was investigated using gene knockout mice. The renal clearance of HCT and furosemide was reduced significantly but not abolished in Mrp4 knockout mice compared with wild-type mice (9.0 ؎ 0.9 versus 15 ؎ 2 ml/min per kg for HCT and 1.9 ؎ 0.3 versus 2.7 ؎ 0.1 ml/min per kg for furosemide), and the amount of HCT that was associated with the kidney specimens was greater in Mrp4 knockout mice (21 ؎ 3 versus 13 ؎ 1 nmol/g kidney). In contrast, Bcrp makes only a negligible contribution because the urinary excretion was unchanged in Bcrp knockout mice. Our results suggest that Mrp4, together with other unknown transporters, accounts for the luminal efflux of HCT and furosemide from proximal tubular epithelial cells.

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“…[10][11][12] Loop and thiazide diuretics must first be secreted by renal proximal tubule cells before reaching their sites of action on the apical membrane. [13][14][15][16] Interactions between diuretics and other secreted drugs, including antibiotics, NSAIDs, antivirals, as well as organic acid in the setting of renal failure, can limit their secretion and natriuretic effects. Kir4.1/5.1 inhibitors that act directly on the basolateral membrane should circumvent this limitation.…”

mentioning

confidence: 99%

Development and Validation of Fluorescence-Based and Automated Patch Clamp–Based Functional Assays for the Inward Rectifier Potassium Channel Kir4.1

RaphemotRene

KadakiaRishin

Olsen

et al. 2013

ASSAY and Drug Development Technologies

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The inward rectifier potassium (Kir) channel Kir4.1 plays essential roles in modulation of neurotransmission and renal sodium transport and may represent a novel drug target for temporal lobe epilepsy and hypertension. The molecular pharmacology of Kir4.1 is limited to neurological drugs, such as fluoxetine (Prozac ª ), exhibiting weak and nonspecific activity toward the channel. The development of potent and selective small-molecule probes would provide critically needed tools for exploring the integrative physiology and therapeutic potential of Kir4.1. A fluorescence-based thallium (Tl + ) flux assay that utilizes a tetracycline-inducible T-Rex-HEK293-Kir4.1 cell line to enable high-throughput screening (HTS) of small-molecule libraries was developed. The assay is dimethyl sulfoxide tolerant and exhibits robust screening statistics (Z 0 = 0.75 -0.06). A pilot screen of 3,655 small molecules and lipids revealed 16 Kir4.1 inhibitors (0.4% hit rate). 3,3-Diphenyl-N-(1-phenylethyl)propan-1-amine, termed VU717, inhibits Kir4.1-mediated thallium flux with an IC 50 of *6 lM. An automated patch clamp assay using the IonFlux HT workbench was developed to facilitate compound characterization. Leak-subtracted ensemble ''loose patch'' recordings revealed robust tetracycline-inducible and Kir4.1 currents that were inhibited by fluoxetine (IC 50 = 10 lM), VU717 (IC 50 = 6 lM), and structurally related calcium channel blocker prenylamine (IC 50 = 6 lM). Finally, we demonstrate that VU717 inhibits Kir4.1 channel activity in cultured rat astrocytes, providing proof-of-concept that the Tl + flux and IonFlux HT assays can enable the discovery of antagonists that are active against native Kir4.1 channels.

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Interactions of Human Organic Anion Transporters with Diuretics

Cited by 184 publications

References 25 publications

Overlapping in vitro and in vivo specificities of the organic anion transporters OAT1 and OAT3 for loop and thiazide diuretics

Overlapping in vitro and in vivo specificities of the organic anion transporters OAT1 and OAT3 for loop and thiazide diuretics

Multidrug Resistance–Associated Protein 4 Is Involved in the Urinary Excretion of Hydrochlorothiazide and Furosemide

Development and Validation of Fluorescence-Based and Automated Patch Clamp–Based Functional Assays for the Inward Rectifier Potassium Channel Kir4.1

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