SLC22A7

更新于：2025-05-07

基本信息

别名

hOAT2、NLT、Novel liver transporter

+ [5]

简介

Functions as a Na(+)-independent bidirectional multispecific transporter (PubMed:11327718, PubMed:18216183, PubMed:21446918, PubMed:28945155). Contributes to the renal and hepatic elimination of endogenous organic compounds from the systemic circulation into the urine and bile, respectively (PubMed:11327718, PubMed:25904762). Capable of transporting a wide range of purine and pyrimidine nucleobases, nucleosides and nucleotides, with cGMP, 2'deoxyguanosine and GMP being the preferred substrates (PubMed:11327718, PubMed:18216183, PubMed:26377792, PubMed:28945155). Functions as a pH- and chloride-independent cGMP bidirectional facilitative transporter that can regulate both intracellular and extracellular levels of cGMP and may be involved in cGMP signaling pathways (PubMed:18216183, PubMed:26377792). Mediates orotate/glutamate bidirectional exchange and most likely display a physiological role in hepatic release of glutamate into the blood (PubMed:21446918). Involved in renal secretion and possible reabsorption of creatinine (PubMed:25904762, PubMed:28945155). Able to uptake prostaglandin E2 (PGE2) and may contribute to PGE2 renal excretion (Probable). Also transports alpha-ketoglutarate and urate (PubMed:11327718, PubMed:26377792). Apart from the orotate/glutamate exchange, the counterions for the uptake of other SLC22A7/OAT2 substrates remain to be identified (PubMed:26377792). Involved in the uptake of prostaglandin F2-alpha (PGF2-alpha). Non functional transporter.

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100 项与 SLC22A7 相关的临床结果

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100 项与 SLC22A7 相关的转化医学

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0 项与 SLC22A7 相关的专利（医药）

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350

项与 SLC22A7 相关的文献（医药）

2025-06-01·Journal of Pharmaceutical Sciences

Progressive amyloid-β accumulation in the brain leads to altered protein expressions in the liver and kidneys of APP knock-in mice

Article

作者: Saito, Takashi ; Iwata, Yumi ; Yagi, Ryotaro ; Masuda, Takeshi ; Uemura, Tatsuki ; Kaneko, Yui ; Ogata, Seiryo ; Ito, Shingo ; Otsuka, Mitsumi ; Ohtsuki, Sumio ; Saido, Takaomi

Impaired hepatic and renal function influence Alzheimer's disease (AD) progression; however, whether AD progression affects these important organ functions remains unclear. Here, we investigated the impact of AD progression, characterized by brain amyloid-beta (Aβ) accumulation, on liver and kidney function of App^{NL-G-F/NL-G-F} (APP-KI) mice using quantitative proteomics. SWATH-based quantitative proteomics revealed changes in mitochondrial, drug metabolism, and pharmacokinetic-related proteins in mouse liver and kidneys during the early (2-month-old) and intermediate (5-month-old) stages of Aβ accumulation. Notably, in 5-month-old APP-KI mouse liver, 25 phase I/II metabolizing enzymes (8 CYPs, 7 UGTs, 7 CESs, and 3 SLCs) and five transporters (2 ABCs and 3 SLCs) were significantly altered; specifically, Ugt1a9 and Slc33a1 protein abundances increased, whereas Ugt1a1 and Abcc3 protein abundances decreased. In the kidneys, 13 phase I/II metabolizing enzymes and 10 ABC-SLC transporters were altered, including Ugt1a6, Ugt1a7, Slc22a7, and Abcb1a. Additionally, plasma proteins, such as albumin and alpha-1-acid glycoprotein, which are critical for drug binding and distribution, were also altered. These results underscore the significant role of progressive brain Aβ accumulation in modifying hepatic and renal protein abundances, potentially influencing drug metabolism and disposition in AD. Our findings provide novel insights into the complex relationship between AD progression and organ dysfunction.

2025-03-01·Drug Metabolism and Disposition

Identification of selective substrates and inhibitors of the major human renal uptake transporters

Article

作者: Warren, Mark S ; Tsang, Yik Pui ; Unadkat, Jashvant D ; Rodriguez, Acilegna G

Renal clearance of drugs mediated by transporters can be affected by diseases (eg, inflammation due to infections), physiological changes (eg, pregnancy), or drug-drug interactions. To elucidate the transporters involved, the magnitude of effect, and the underlying mechanisms, human proximal tubular epithelial cells could be exposed to potential perpetrators (eg, cytokines, pregnancy-related hormones or the interacting drug), and the activity of transporters quantified. A crucial prerequisite for such studies is the identification of selective substrates or substrate-inhibitor pairs for each renal transporter. Using transporter-transfected mammalian cells and membrane vesicles, we systematically evaluated the selectivity of 6 substrates (or substrate-inhibitor pairs) for the major uptake and efflux renal transporters. Cidofovir, levocetirizine, and ergothioneine were found to be selective substrates of the organic anion transporter (OAT) 1, 4, and organic cation/carnitine transporter 1, respectively. Nicotinic acid was transported by OAT2, but also by OAT1 and 3, though to a lesser extent. Probenecid did not selectively inhibit OAT1/3-mediated uptake of nicotinic acid, but quercetin did, allowing selective measurement of OAT2 activity. Interestingly, nicotinic acid was also transported by the endogenous monocarboxylate transporter 1 in HEK293 cells. Glycochenodeoxycholic acid sulfate was transported by OAT3 and multidrug resistance-associated protein 2 (MRP2), with MRP2 selectively inhibited by cyclosporine A, allowing selective measurement of OAT3 activity. Atenolol was transported by organic cation transporter 2 and multidrug and toxin extrusion proteins 1 and 2-K, with multidrug and toxin extrusion proteins activity selectively inhibited by mitoxantrone, allowing selective measurement of organic cation transporter 2 activity. SIGNIFICANCE STATEMENT: These findings provide a framework for measuring the in vitro activity of individual uptake transporters in primary human proximal tubular epithelial cells. By applying our proposed methodology, researchers can quantify how various factors (eg, cytokines, pregnancy-related hormone, drug interactions) modulate individual renal uptake transporter activity in proximal tubular epithelial cells.

2025-01-01·European Journal of Drug Metabolism and Pharmacokinetics

Hypertensive Nephropathy Changes the Expression of Drug-Metabolizing Enzymes and Transporters in Spontaneously Hypertensive Rat Liver and Kidney

Article

作者: Pan, Yueqing ; Liu, Menghua ; Wei, Minlong ; Zou, Wei ; Yang, Zhuan ; Gan, Yulin

BACKGROUND AND OBJECTIVESHypertensive nephropathy (HN) has become one of the main causes of end-stage renal disease. Drug combination therapy is a common clinical treatment for HN. However, the impact of HN on drug-metabolizing enzymes and transporters, which may lead to drug-drug interactions (DDIs) and even trigger toxic side effects, remains unclear. The aim of this study was to investigate changes in major drug-metabolizing enzymes and transporters in the liver and kidney of HN rats to improve the scientific foundations for the clinical treatment of HN.METHODSSpontaneously hypertensive rats (SHRs) were used as an animal HN model because their hypertension is similar to that of humans. Wistar-Kyoto rats (WKYs) were used as the control group. Body weight, blood pressure, hematoxylin-eosin (HE) staining and biochemical analysis were performed to evaluate whether the HN model was successfully constructed. Quantitative real-time polymerase chain reaction (PCR) and western blotting were used to evaluate the mRNA and protein expression of drug-metabolizing enzymes, transporters and related nuclear transcription factors.RESULTSIn HN rats, the mRNA expression of the drug-metabolizing enzymes cytochrome P450 (Cyp) 2b1, Cyp2c11, Cyp3a1 and Cyp7a1 was significantly upregulated. The protein level of CYP3A1 was consistent with its mRNA expression. Interestingly, the mRNA expression of the hepatic transporters organic cation transporter (Oct) 1, Oct2, organic anion transporter (Oat) 1, Oat2, multidrug resistant protein (Mrp) 2, multidrug resistance (Mdr) 1, organic anion transporting polypeptide (Oatp) 1b2 and na+/taurocholate cotransporting polypeptide (Ntcp) was also markedly upregulated. This may be directly influenced by the upregulation of the expression of the nuclear receptors farnesoid X receptor (Fxr), pregnane X receptor (Pxr), liver X-activated receptor (Lxr) and constitutive androstane receptor (Car). In the kidney of HN rats, the mRNA level of the drug-metabolizing enzyme Cyp2b1 significantly increased, while levels of Cyp1a1, Cyp2c11, Cyp3a1 and Cyp3a2 did not significantly change. The mRNA expression of the transporters multidrug and toxin extrusion (Mate) 1 and Mrp2 was obviously increased but was markedly depressed for peptide transporters (Pept) 1 and Pept2. These changes may be related to the cross effects of Pxr, Fxr and Car in kidney.CONCLUSIONHN pathological status can alter the expression of drug-metabolizing enzymes and transporters in the liver and kidney to varying degrees, thus affecting the disposition of substrate drugs in vivo. This suggests that to avoid potential risks, caution should be exercised when administering combination therapy for HN treatment.

项与 SLC22A7 相关的新闻（医药）

2021-11-09

·BioSpace

BioIVT to Showcase Use of a Sandwich-cultured Human Hepatocyte Model to Study Drug-Drug Interactions

Researchers will describe how they used a transporter-competent SCHH model to investigate the DDI potential of bempedoic acid, a drug indicated for hypercholesterolemia Westbury, NY – November 9, 2021 – BioIVT, a leading provider of research models and services for drug and diagnostic development, is hosting a webinar in which researchers will discuss how they used a sandwich-cultured human hepatocyte (SCHH) model to investigate the drug-drug interaction (DDI) potential of bempedoic acid, a drug that was recently approved to treat hypercholesterolemia. This online event will be held at 11 a.m. ET on November 11. “We are excited to have this opportunity to highlight some of the important DDI research we implemented,” said Dr. Kenneth R. Brouwer, Vice President of ADME-Tox at BioIVT. “BioIVT scientists collaborated with colleagues from Esperion Therapeutics, Inc., the University of Washington in Seattle, and Western University in London, Ontario on this project.” During phase 2 and 3 trials of bempedoic acid, small, reversible increases in serum creatinine and uric acid levels were observed.1 Ensuing in vitro studies showed that bempedoic acid inhibits OAT2-mediated transport of uric acid, creatinine, and cGMP8 with a wide range of potencies.1 But it was unknown whether bempedoic acid would inhibit OAT2-mediated transport in the liver. To better understand the pharmacokinetics of bempedoic acid disposition, BioIVT designed a study to investigate the drug’s effect on the hepatic disposition of warfarin and naproxen, two well-characterized OAT2 substrates. To ensure in vivo relevant transporter function, TRANSPORTER CERTIFIED® hepatocytes were used in a SCHH model. Warfarin was chosen because it tends to be involved in significant DDIs, it is reportedly dependent on OAT2 for uptake, and hepatic metabolism for clearance. Naproxen was selected as a negative control because results from in human hepatocyte studies have indicated there is no OAT2-mediated hepatic uptake despite contrary findings in in vitro studies in overexpressing systems.1 As part of its comprehensive portfolio of ADME-Tox research services, BioIVT designs and implements programs to help clients with lead selection and optimization, IND submissions, and address mechanistic questions raised during clinical development. Dr. Maurice Emery, Executive Director at Esperion Therapeutics, will review the results of this SCHH study during the webinar and discuss their potential clinical implications. Dr. Kenneth Brouwer will discuss how the SCHH model functions as a “whole-cell” system, which can improve the in-vitro in-vivo correlation of transporter-mediated hepatic disposition. Additional information about this complimentary event is available at . Reference 24th North American ISSX Meeting Poster: Effect of Bempedoic Acid on Warfarin and Naproxen In Vitro Disposition in Sandwich-Cultured Human Hepatocytes (SCHH). Sept. 16, 2021. About BioIVT BioIVT is a leading global provider of research models and value-added research services for drug discovery and development. We specialize in control and disease-state biospecimens including human and animal tissues, cell products, blood and other biofluids. Our unmatched portfolio of clinical specimens directly supports precision medicine research and the effort to improve patient outcomes by coupling comprehensive clinical data with donor samples. And as the premier supplier of hepatic products, including hepatocytes and subcellular fractions, BioIVT enables scientists to better understand the pharmacokinetics and drug metabolism of newly discovered compounds and their effects on disease processes. By combining our technical expertise, exceptional customer service, and unparalleled access to biological specimens, BioIVT serves the research community as a trusted partner in elevating science. For more information, please visit or follow the company on Twitter @BioIVT.

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