Your search keyword '"Stephen H. Wright"' showing total 169 results

1. Predicting disruptions to drug pharmacokinetics and the risk of adverse drug reactions in non-alcoholic steatohepatitis patients

Author

Solène Marie, Kayla L. Frost, Raymond K. Hau, Lucy Martinez-Guerrero, Jailyn M. Izu, Cassandra M. Myers, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Non-alcoholic steatohepatitis, Hepatic elimination, Transporter, Enzyme, Pharmacokinetics, Drug–drug interaction, Therapeutics. Pharmacology, RM1-950

Abstract

The liver plays a central role in the pharmacokinetics of drugs through drug metabolizing enzymes and transporters. Non-alcoholic steatohepatitis (NASH) causes disease-specific alterations to the absorption, distribution, metabolism, and excretion (ADME) processes, including a decrease in protein expression of basolateral uptake transporters, an increase in efflux transporters, and modifications to enzyme activity. This can result in increased drug exposure and adverse drug reactions (ADRs). Our goal was to predict drugs that pose increased risks for ADRs in NASH patients. Bibliographic research identified 71 drugs with reported ADRs in patients with liver disease, mainly non-alcoholic fatty liver disease (NAFLD), 54 of which are known substrates of transporters and/or metabolizing enzymes. Since NASH is the progressive form of NAFLD but is most frequently undiagnosed, we identified other drugs at risk based on NASH-specific alterations to ADME processes. Here, we present another list of 71 drugs at risk of pharmacokinetic disruption in NASH, based on their transport and/or metabolism processes. It encompasses drugs from various pharmacological classes for which ADRs may occur when used in NASH patients, especially when eliminated through multiple pathways altered by the disease. Therefore, these results may inform clinicians regarding the selection of drugs for use in NASH patients.

Published

2023

2. PF‐07321332 (Nirmatrelvir) does not interact with human ENT1 or ENT2: Implications for COVID‐19 patients

Author

Raymond K. Hau, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Therapeutics. Pharmacology, RM1-950, Public aspects of medicine, RA1-1270

Abstract

Abstract The ongoing pandemic of severe acute respiratory syndrome‐coronavirus 2 (SARS‐CoV‐2) and subsequently, coronavirus disease 2019 (COVID‐19), has led to the deaths of over 6.1 million people and sparked a greater interest in virology to expedite the development process for antivirals. The US Food and Drug Administration (FDA) granted emergency use authorization for three antivirals: remdesivir, molnupiravir, and nirmatrelvir. Remdesivir and molnupiravir are nucleoside analogs that undergo biotransformation to form active metabolites that incorporate into new viral RNA to stall replication. Unlike remdesivir or molnupiravir, nirmatrelvir is a protease inhibitor that covalently binds to the SARS‐CoV‐2 3C‐like protease to interrupt the viral replication cycle. A recent study identified that remdesivir and the active metabolite of molnupiravir, EIDD‐1931, are substrates of equilibrative nucleoside transporters 1 and 2 (ENT1 and 2). Despite the ubiquitous expression of the ENTs, the preclinical efficacy of remdesivir and molnupiravir is not reflected in wide‐scale SARS‐CoV‐2 clinical trials. Interestingly, downregulation of ENT1 and ENT2 expression has been shown in lung epithelial and endothelial cells in response to hypoxia and acute lung injury, although it has not been directly studied in patients with COVID‐19. It is possible that the poor efficacy of remdesivir and molnupiravir in these patients may be partially attributed to the repression of ENTs in the lungs, but further studies are warranted. This study investigated the interaction between nirmatrelvir and the ENTs and found that it was a poor inhibitor of ENT‐mediated [3H]uridine uptake at 300 μM. Unlike for remdesivir or EIDD‐1931, ENT activity is unlikely to be a factor for nirmatrelvir disposition in humans; however, whether this contributes to the similar in vitro and clinical efficacy will require further mechanistic studies.

Published

2022

3. Testicular disposition of clofarabine in rats is dependent on equilibrative nucleoside transporters

Author

Siennah R. Miller, Joseph L. Jilek, Meghan E. McGrath, Raymond K. Hau, Erin Q. Jennings, James J. Galligan, Stephen H. Wright, and Nathan J. Cherrington

Subjects

blood‐testis barrier, clofarabine, nucleoside transporter, nucleosides, Sertoli cells, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Acute lymphoblastic leukemia (ALL) is the most common cancer in children and adolescents. Although the 5‐year survival rate is high, some patients respond poorly to chemotherapy or have recurrence in locations such as the testis. The blood–testis barrier (BTB) can prevent complete eradication by limiting chemotherapeutic access and lead to testicular relapse unless a chemotherapeutic is a substrate of drug transporters present at this barrier. Equilibrative nucleoside transporter (ENT) 1 and ENT2 facilitate the movement of substrates across the BTB. Clofarabine is a nucleoside analog used to treat relapsed or refractory ALL. This study investigated the role of ENTs in the testicular disposition of clofarabine. Pharmacological inhibition of the ENTs by 6‐nitrobenzylthioinosine (NBMPR) was used to determine ENT contribution to clofarabine transport in primary rat Sertoli cells, in human Sertoli cells, and across the rat BTB. The presence of NBMPR decreased clofarabine uptake by 40% in primary rat Sertoli cells (p = .0329) and by 53% in a human Sertoli cell line (p = .0899). Rats treated with 10 mg/kg intraperitoneal (IP) injection of the NBMPR prodrug, 6‐nitrobenzylthioinosine 5′‐monophosphate (NBMPR‐P), or vehicle, followed by an intravenous (IV) bolus 10 mg/kg dose of clofarabine, showed a trend toward a lower testis concentration of clofarabine than vehicle (1.81 ± 0.59 vs. 2.65 ± 0.92 ng/mg tissue; p = .1160). This suggests that ENTs could be important for clofarabine disposition. Clofarabine may be capable of crossing the human BTB, and its potential use as a first‐line treatment to avoid testicular relapse should be considered.

Published

2021

4. Generation of a hTERT-Immortalized Human Sertoli Cell Model to Study Transporter Dynamics at the Blood-Testis Barrier

Author

Raymond K. Hau, Siennah R. Miller, Stephen H. Wright, and Nathan J. Cherrington

Subjects

cell immortalization, sertoli cell, blood–testis barrier, testes, xenobiotic transporter, drug disposition, Pharmacy and materia medica, RS1-441

Abstract

The blood-testis barrier (BTB) formed by adjacent Sertoli cells (SCs) limits the entry of many chemicals into seminiferous tubules. Differences in rodent and human substrate-transporter selectivity or kinetics can misrepresent conclusions drawn using rodent in vitro models. Therefore, human in vitro models are preferable when studying transporter dynamics at the BTB. This study describes a hTERT-immortalized human SC line (hT-SerC) with significantly increased replication capacity and minor phenotypic alterations compared to primary human SCs. Notably, hT-SerCs retained similar morphology and minimal changes to mRNA expression of several common SC genes, including AR and FSHR. The mRNA expression of most xenobiotic transporters was within the 2-fold difference threshold in RT-qPCR analysis with some exceptions (OAT3, OCT3, OCTN1, OATP3A1, OATP4A1, ENT1, and ENT2). Functional analysis of the equilibrative nucleoside transporters (ENTs) revealed that primary human SCs and hT-SerCs predominantly express ENT1 with minimal ENT2 expression at the plasma membrane. ENT1-mediated uptake of [3H] uridine was linear over 10 min and inhibited by NBMPR with an IC50 value of 1.35 ± 0.37 nM. These results demonstrate that hT-SerCs can functionally model elements of transport across the human BTB, potentially leading to identification of other transport pathways for xenobiotics, and will guide drug discovery efforts in developing effective BTB-permeable compounds.

Published

2020

5. Transporter Inhibition Profile for the Antivirals Tilorone, Quinacrine and Pyronaridine

Author

Patricia A. Vignaux, Thomas R. Lane, Ana C. Puhl, Raymond K. Hau, Stephen H. Wright, Nathan J. Cherrington, and Sean Ekins

Subjects

General Chemical Engineering, General Chemistry

Published

2023

6. Drug Transporters at the Human Blood-Testis Barrier

Author

Raymond K. Hau, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Pharmaceutical Science

Published

2023

7. Machine Learning Models Identify New Inhibitors for Human OATP1B1

Author

Thomas R. Lane, Fabio Urbina, Xiaohong Zhang, Margret Fye, Jacob Gerlach, Stephen H. Wright, and Sean Ekins

Subjects

Machine Learning, Cricetulus, Support Vector Machine, Cricetinae, Drug Discovery, Animals, Humans, Pharmaceutical Science, Molecular Medicine, Bayes Theorem, Algorithms, Software

Abstract

The uptake transporter OATP1B1 (SLC01B1) is largely localized to the sinusoidal membrane of hepatocytes and is a known victim of unwanted drug-drug interactions. Computational models are useful for identifying potential substrates and/or inhibitors of clinically relevant transporters. Our goal was to generate OATP1B1 in vitro inhibition data for [

Published

2022

8. Attenuated Ochratoxin A Transporter Expression in a Mouse Model of Nonalcoholic Steatohepatitis Protects against Proximal Convoluted Tubule Toxicity

Author

Joseph L. Jilek, Kayla L. Frost, Solène Marie, Cassandra M. Myers, Michael Goedken, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Disease Models, Animal, Mice, Non-alcoholic Fatty Liver Disease, Animals, Humans, Organic Anion Transporters, Protein Isoforms, Pharmaceutical Science, Mycotoxins, Thioacetamide, Kidney, Ochratoxins

Abstract

Ochratoxin A (OTA) is an abundant mycotoxin, yet the toxicological impact of its disposition is not well studied. OTA is an organic anion transporter (OAT) substrate primarily excreted in urine despite a long half-life and extensive protein binding. Altered renal transporter expression during disease, including nonalcoholic steatohepatitis (NASH), may influence response to OTA exposure, but the impact of NASH on OTA toxicokinetics, tissue distribution, and associated nephrotoxicity is unknown. By inducing NASH in fast food-dieted/thioacetamide-exposed mice, we evaluated the effect of NASH on a bolus OTA exposure (12.5 mg/kg by mouth) after 3 days. NASH mice presented with less gross toxicity (44% less body weight loss), and kidney and liver weights of NASH mice were 11% and 24% higher, respectively, than healthy mice. Organ and body weight changes coincided with reduced renal proximal tubule cells vacuolation, degeneration, and necrosis, though no OTA-induced hepatic lesions were found. OTA systemic exposure in NASH mice increased modestly from 5.65 ± 1.10 to 7.95 ± 0.61 mg*h/ml per kg BW, and renal excretion increased robustly from 5.55% ± 0.37% to 13.11% ± 3.10%, relative to healthy mice. Total urinary excretion of OTA increased from 24.41 ± 1.74 to 40.07 ± 9.19

Published

2021

9. Renal Transporter Alterations in Patients with Chronic Liver Diseases: Nonalcoholic Steatohepatitis, Alcohol-associated, Viral Hepatitis, and Alcohol-Viral Combination

Author

Kayla L. Frost, Joseph L. Jilek, Shripad Sinari, Robert R. Klein, Dean Billheimer, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Pharmaceutical Science

Abstract

Alterations in hepatic transporters have been identified in pre-cirrhotic chronic liver diseases (CLD) that result in pharmacokinetic variations causing adverse drug reactions (ADRs). However, the effect of CLD on the expression of renal transporters is unknown despite the overwhelming evidence of kidney injury in CLD patients. This study determines the transcriptomic and proteomic expression profiles of renal drug transporters in patients with defined CLD etiology. Renal biopsies were obtained from patients with a history of CLD etiologies, including nonalcoholic fatty liver disease (NAFLD), nonalcoholic steatohepatitis (NASH), alcohol-associated liver disease (ALD), viral hepatitis C (HCV), and combination ALD/HCV. A significant decrease in organic anion transporter 3 (OAT3) was identified in NASH, ALD, HCV, and ALD/HCV (1.56{plus minus} 1.10; 1.01{plus minus} 0.46; 1.03{plus minus} 0.43; 0.86{plus minus} 0.57 pmol/mg protein) relative to control (2.77{plus minus} 1.39 pmol/mg protein). Additionally, a decrease was shown for OAT4 in NASH (24.9{plus minus} 5.69 pmol/mg protein) relative to control (43.8{plus minus} 19.9 pmol/mg protein) and in urate transporter 1 (URAT1) for ALD and HCV (1.56{plus minus} 0.15 and 1.65{plus minus} 0.69 pmol/mg protein) relative to control (4.69{plus minus} 4.59 pmol/mg protein). These decreases in organic anion transporter expression could result in increased and prolonged systemic exposure to drugs and possible toxicity. Renal transporter changes, in addition to hepatic transporter alterations should be considered in dose adjustments for CLD patients for a more accurate disposition profile. It is important to consider a multi-organ approach to altered pharmacokinetics of drugs prescribed to CLD patients to prevent ADRs and improve patient outcomes.

Published

2022

10. Remdesivir and EIDD-1931 Interact with Human Equilibrative Nucleoside Transporters 1 and 2: Implications for Reaching SARS-CoV-2 Viral Sanctuary Sites

Author

Meghan E. McGrath, Sean Ekins, Nathan J. Cherrington, Kimberley M. Zorn, Stephen H. Wright, and Siennah R. Miller

Subjects

medicine.drug_class, Cytidine, Pharmacology, Antiviral Agents, Equilibrative Nucleoside Transporter 1, chemistry.chemical_compound, medicine, Humans, Drug Interactions, Equilibrative-Nucleoside Transporter 2, IC50, Active metabolite, Alanine, Dose-Response Relationship, Drug, Nucleoside analogue, SARS-CoV-2, Chemistry, COVID-19, Transporter, Articles, Adenosine Monophosphate, In vitro, Uridine, COVID-19 Drug Treatment, Molecular Medicine, Antiviral drug, Nucleoside, HeLa Cells, Protein Binding, medicine.drug

Abstract

Equilibrative nucleoside transporters (ENTs) are present at the blood-testis barrier (BTB), where they can facilitate antiviral drug disposition to eliminate a sanctuary site for viruses detectable in semen. The purpose of this study was to investigate ENT-drug interactions with three nucleoside analogs, remdesivir, molnupiravir, and molnupiravir’s active metabolite, β-d-N(4)-hydroxycytidine (EIDD-1931), and four non-nucleoside molecules repurposed as antivirals for coronavirus disease 2019 (COVID-19). The study used three-dimensional pharmacophores for ENT1 and ENT2 substrates and inhibitors and Bayesian machine learning models to identify potential interactions with these transporters. In vitro transport experiments demonstrated that remdesivir was the most potent inhibitor of ENT-mediated [(3)H]uridine uptake (ENT1 IC(50): 39 μM; ENT2 IC(50): 77 μM), followed by EIDD-1931 (ENT1 IC(50): 259 μM; ENT2 IC(50): 467 μM), whereas molnupiravir was a modest inhibitor (ENT1 IC(50): 701 μM; ENT2 IC(50): 851 μM). Other proposed antivirals failed to inhibit ENT-mediated [(3)H]uridine uptake below 1 mM. Remdesivir accumulation decreased in the presence of 6-S-[(4-nitrophenyl)methyl]-6-thioinosine (NBMPR) by 30% in ENT1 cells (P = 0.0248) and 27% in ENT2 cells (P = 0.0054). EIDD-1931 accumulation decreased in the presence of NBMPR by 77% in ENT1 cells (P = 0.0463) and by 64% in ENT2 cells (P = 0.0132), which supported computational predictions that both are ENT substrates that may be important for efficacy against COVID-19. NBMPR failed to decrease molnupiravir uptake, suggesting that ENT interaction is likely inhibitory. Our combined computational and in vitro data can be used to identify additional ENT-drug interactions to improve our understanding of drugs that can circumvent the BTB. SIGNIFICANCE STATEMENT: This study identified remdesivir and EIDD-1931 as substrates of equilibrative nucleoside transporters 1 and 2. This provides a potential mechanism for uptake of these drugs into cells and may be important for antiviral potential in the testes and other tissues expressing these transporters.

Published

2021

11. Cationic Compounds with SARS-CoV-2 Antiviral Activity and Their Interaction with Organic Cation Transporter/Multidrug and Toxin Extruder Secretory Transporters

Author

Xiaohong Zhang, Sean Ekins, Kimberley M. Zorn, Stephen H. Wright, and Lucy J. Martinez-Guerrero

Subjects

Organic Cation Transport Proteins, Cetylpyridinium, CHO Cells, Tilorone, Antiviral Agents, Cricetulus, Cricetinae, medicine, Animals, Secretion, Naphthyridines, IC50, Secretory pathway, Pharmacology, Organic cation transport proteins, biology, SARS-CoV-2, Chemistry, Chinese hamster ovary cell, Chloroquine, Transporter, In vitro, Metabolism, Transport, and Pharmacogenetics, Biochemistry, Quinacrine, biology.protein, Molecular Medicine, Benzalkonium Compounds, medicine.drug

Abstract

In the wake of the COVID-19 pandemic, drug repurposing has been highlighted for rapid introduction of therapeutics. Proposed drugs with activity against SARS-CoV-2 include compounds with positive charges at physiologic pH, making them potential targets for the organic cation secretory transporters of kidney and liver, i.e., the basolateral organic cation transporters, OCT1 and OCT2; and the apical multidrug and toxin extruders, MATE1 and MATE2-K. We selected several compounds proposed to have in vitro activity against SARS-CoV-2 (chloroquine, hydroxychloroquine, quinacrine, tilorone, pyronaridine, cetylpyridinium, and miramistin) to test their interaction with OCT and MATE transporters. We used Bayesian machine learning models to generate predictions for each molecule with each transporter and also experimentally determined IC(50) values for each compound against labeled substrate transport into CHO cells that stably expressed OCT2, MATE1, or MATE2-K using three structurally distinct substrates (atenolol, metformin and 1-methyl-4-phenylpyridinium) to assess the impact of substrate structure on inhibitory efficacy. For the OCTs substrate identity influenced IC(50) values, although the effect was larger and more systematic for OCT2. In contrast, inhibition of MATE1-mediated transport was largely insensitive to substrate identity. Unlike MATE1, inhibition of MATE2-K was influenced, albeit modestly, by substrate identity. Maximum unbound plasma concentration/IC(50) ratios were used to identify potential clinical DDI recommendations; all the compounds interacted with the OCT/MATE secretory pathway, most with sufficient avidity to represent potential DDI issues for secretion of cationic drugs. This should be considered when proposing cationic agents as repurposed antivirals. SIGNIFICANCE STATEMENT: Drugs proposed as potential COVID-19 therapeutics based on in vitro activity data against SARS-CoV-2 include compounds with positive charges at physiological pH, making them potential interactors with the OCT/MATE renal secretory pathway. We tested seven such molecules as inhibitors of OCT1/2 and MATE1/2-K. All the compounds blocked transport activity regardless of substrate used to monitor activity. Suggesting that plasma concentrations achieved by normal clinical application of the test agents could be expected to influence the pharmacokinetics of selected cationic drugs.

Published

2021

12. Multiple Computational Approaches for Predicting Drug Interactions with Human Equilibrative Nucleoside Transporter 1

Author

Kimberley M. Zorn, Nathan J. Cherrington, Sean Ekins, Stephen H. Wright, Thomas R. Lane, and Siennah R. Miller

Subjects

Drug, media_common.quotation_subject, Pharmaceutical Science, Pharmacology, Equilibrative nucleoside transporter 1, Equilibrative Nucleoside Transporter 1, Thioinosine, Ribavirin, medicine, Humans, Drug Interactions, Darunavir, media_common, Mizoribine, biology, Chemistry, Drug discovery, Nucleosides, Transporter, Articles, biology.protein, Ribonucleosides, Pharmacophore, Nucleoside, HeLa Cells, medicine.drug

Abstract

Equilibrativenucleoside transporters (ENTs) participate in the pharmacokinetics and disposition of nucleoside analog drugs. Understanding drug interactions with the ENTs may inform and facilitate the development of new drugs, including chemotherapeutics and antivirals that require access to sanctuary sites such as the male genital tract. This study created three-dimensional pharmacophores for ENT1 and ENT2 substrates and inhibitors using K(t) and IC(50) data curated from the literature. Substrate pharmacophores for ENT1 and ENT2 are distinct, with partial overlap of hydrogen bond donors, whereas the inhibitor pharmacophores predominantly feature hydrogen bond acceptors. Mizoribine and ribavirin mapped to the ENT1 substrate pharmacophore and proved to be substrates of the ENTs. The presence of the ENT-specific inhibitor 6-S-[(4-nitrophenyl)methyl]-6-thioinosine (NBMPR) decreased mizoribine accumulation in ENT1 and ENT2 cells (ENT1, ∼70% decrease, P = 0.0046; ENT2, ∼50% decrease, P = 0.0012). NBMPR also decreased ribavirin accumulation in ENT1 and ENT2 cells (ENT1: ∼50% decrease, P = 0.0498; ENT2: ∼30% decrease, P = 0.0125). Darunavir mapped to the ENT1 inhibitor pharmacophore and NBMPR did not significantly influence darunavir accumulation in either ENT1 or ENT2 cells (ENT1: P = 0.28; ENT2: P = 0.53), indicating that darunavir’s interaction with the ENTs is limited to inhibition. These computational and in vitro models can inform compound selection in the drug discovery and development process, thereby reducing time and expense of identification and optimization of ENT-interacting compounds. SIGNIFICANCE STATEMENT: This study developed computational models of human equilibrative nucleoside transporters (ENTs) to predict drug interactions and validated these models with two compounds in vitro. Identification and prediction of ENT1 and ENT2 substrates allows for the determination of drugs that can penetrate tissues expressing these transporters.

Published

2021

13. InVitroandInVivoModels for Drug Transport Across the Blood-Testis Barrier

Author

Raymond K. Hau, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Pharmaceutical Science

Published

2023

14. Localization of Xenobiotic Transporters Expressed at the Human Blood-Testis Barrier

Author

Raymond K. Hau, Robert R. Klein, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Male, Cations, Organic Cation Transporter 1, Pharmaceutical Science, Humans, Articles, Blood-Testis Barrier, Xenobiotics

Abstract

The blood-testis barrier (BTB) is formed by basal tight junctions between adjacent Sertoli cells (SCs) of the seminiferous tubules and acts as a physical barrier to protect developing germ cells in the adluminal compartment from reproductive toxicants. Xenobiotics, including antivirals, male contraceptives, and cancer chemotherapeutics, are known to cross the BTB, although the mechanisms that permit barrier circumvention are generally unknown. This study used immunohistological staining of human testicular tissue to determine the site of expression for xenobiotic transporters that facilitate transport across the BTB. Organic anion transporter (OAT) 1, OAT2, and organic cation transporter, novel (OCTN) 1 primarily localized to the basal membrane of SCs, whereas OCTN2, multidrug resistance protein (MRP) 3, MRP6, and MRP7 localized to SC basal membranes and peritubular myoid cells (PMCs) surrounding the seminiferous tubules. Concentrative nucleoside transporter (CNT) 2 localized to Leydig cells (LCs), PMCs, and SC apicolateral membranes. Organic cation transporter (OCT) 1, OCT2, and OCT3 mostly localized to PMCs and LCs, although there was minor staining in developing germ cells for OCT3. Organic anion transporting polypeptide (OATP) 1A2, OATP1B1, OATP1B3, OATP2A1, OATP2B1, and OATP3A1-v2 localized to SC basal membranes with diffuse staining for some transporters. Notably, OATP1C1 and OATP4A1 primarily localized to LCs. Positive staining for multidrug and toxin extrusion protein (MATE) 1 was only observed throughout the adluminal compartment. Definitive staining for CNT1, OAT3, MATE2, and OATP6A1 was not observed. The location of these transporters is consistent with their involvement in the movement of xenobiotics across the BTB. Altogether, the localization of these transporters provides insight into the mechanisms of drug disposition across the BTB and will be useful in developing tools to overcome the pharmacokinetic and pharmacodynamic difficulties presented by the BTB. SIGNIFICANCE STATEMENT: Although the total mRNA and protein expression of drug transporters in the testes has been explored, the localization of many transporters at the blood-testis barrier (BTB) has not been determined. This study applied immunohistological staining in human testicular tissues to identify the cellular localization of drug transporters in the testes. The observations made in this study have implications for the development of drugs that can effectively use transporters expressed at the basal membranes of Sertoli cells to bypass the BTB.

Published

2022

15. Predicting Drug Interactions with Human Equilibrative Nucleoside Transporters 1 and 2 Using Functional Knockout Cell Lines and Bayesian Modeling

Author

Kimberley M. Zorn, Joseph L. Jilek, Xiaohong Zhang, Raymond K. Hau, Siennah R. Miller, Erin Q. Jennings, Sean Ekins, Daniel H. Foil, Nathan J. Cherrington, James J. Galligan, and Stephen H. Wright

Subjects

0301 basic medicine, Ticagrelor, Uridine Triacetate, Acetates, Transport Pathway, Cell Line, Equilibrative Nucleoside Transporter 1, Machine Learning, Gene Knockout Techniques, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Thioinosine, Humans, Drug Interactions, Equilibrative-Nucleoside Transporter 2, Nevirapine, Uridine, Gene knockout, Uridine transport, Pharmacology, Chemistry, Bayes Theorem, Biological Transport, Equilibrative nucleoside transporter, Transporter, Articles, Dideoxynucleosides, 030104 developmental biology, Biochemistry, Molecular Medicine, CRISPR-Cas Systems, Nucleoside, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Equilibrative nucleoside transporters (ENTs) 1 and 2 facilitate nucleoside transport across the blood-testis barrier (BTB). Improving drug entry into the testes with drugs that use endogenous transport pathways may lead to more effective treatments for diseases within the reproductive tract. In this study, CRISPR/CRISPR-associated protein 9 was used to generate HeLa cell lines in which ENT expression was limited to ENT1 or ENT2. We characterized uridine transport in these cell lines and generated Bayesian models to predict interactions with the ENTs. Quantification of [(3)H]uridine uptake in the presence of the ENT-specific inhibitor S-(4-nitrobenzyl)-6-thioinosine (NBMPR) demonstrated functional loss of each transporter. Nine nucleoside reverse-transcriptase inhibitors and 37 nucleoside/heterocycle analogs were evaluated to identify ENT interactions. Twenty-one compounds inhibited uridine uptake and abacavir, nevirapine, ticagrelor, and uridine triacetate had different IC(50) values for ENT1 and ENT2. Total accumulation of four identified inhibitors was measured with and without NBMPR to determine whether there was ENT-mediated transport. Clofarabine and cladribine were ENT1 and ENT2 substrates, whereas nevirapine and lexibulin were ENT1 and ENT2 nontransported inhibitors. Bayesian models generated using Assay Central machine learning software yielded reasonably high internal validation performance (receiver operator characteristic > 0.7). ENT1 IC(50)-based models were generated from ChEMBL; subvalidations using this training data set correctly predicted 58% of inhibitors when analyzing activity by percent uptake and 63% when using estimated-IC(50) values. Determining drug interactions with these transporters can be useful in identifying and predicting compounds that are ENT1 and ENT2 substrates and can thereby circumvent the BTB through this transepithelial transport pathway in Sertoli cells. SIGNIFICANCE STATEMENT: This study is the first to predict drug interactions with equilibrative nucleoside transporter (ENT) 1 and ENT2 using Bayesian modeling. Novel CRISPR/CRISPR-associated protein 9 functional knockouts of ENT1 and ENT2 in HeLa S3 cells were generated and characterized. Determining drug interactions with these transporters can be useful in identifying and predicting compounds that are ENT1 and ENT2 substrates and can circumvent the blood-testis barrier through this transepithelial transport pathway in Sertoli cells.

Published

2020

16. Physiological Characterization of the Transporter-Mediated Uptake of the Reversible Male Contraceptive H2-Gamendazole Across the Blood-Testis Barrier

Author

Raymond K. Hau, Joseph S. Tash, Gunda I. Georg, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Male, Indazoles, Carboxylic Acids, Contraceptive Agents, Male, Membrane Transport Proteins, Organic Anion Transporters, CHO Cells, Cricetulus, Dogs, HEK293 Cells, Tandem Mass Spectrometry, Cricetinae, Molecular Medicine, Animals, Humans, Female, Blood-Testis Barrier, Chromatography, Liquid

Abstract

The blood-testis barrier (BTB) is formed by a tight network of Sertoli cells (SCs) to limit the movement of reproductive toxicants from the blood into the male genital tract. Transporters expressed at the basal membranes of SCs also influence the disposition of drugs across the BTB. The reversible, nonhormonal contraceptive, H2-gamendazole (H2-GMZ), is an indazole carboxylic acid analog that accumulates over 10 times more in the testes compared with other organs. However, the mechanism(s) by which H2-GMZ circumvents the BTB are unknown. This study describes the physiologic characteristics of the carrier-mediated process(es) that permit H2-GMZ and other analogs to penetrate SCs. Uptake studies were performed using an immortalized human SC line (hT-SerC) and liquid chromatography-tandem mass spectrometry (LC-MS/MS). Uptake of H2-GMZ and four analogs followed Michaelis-Menten transport kinetics (one analog exhibited poor penetration). H2-GMZ uptake was strongly inhibited by indomethacin, diclofenac, MK-571, and several analogs. Moreover, H2-GMZ uptake was stimulated by an acidic extracellular pH, reduced at basic pHs, and independent of extracellular Na

Published

2022

17. Transport Turnover Rates for Human OCT2 and MATE1 Expressed in Chinese Hamster Ovary Cells

Author

Xiaohong Zhang and Stephen H. Wright

Subjects

kidney, Organic Cation Transport Proteins, QH301-705.5, Organic Chemistry, Gene Expression, Organic Cation Transporter 2, General Medicine, CHO Cells, Catalysis, Computer Science Applications, Inorganic Chemistry, Chemistry, Protein Transport, Cricetulus, transporter turnover rate, transport, Animals, Humans, organic cation, Physical and Theoretical Chemistry, Biology (General), Molecular Biology, QD1-999, Spectroscopy

Abstract

MATE1 (multidrug and toxin extruder 1) and OCT2 (organic cation transporter 2) play critical roles in organic cation excretion by the human kidney. The transporter turnover rate (TOR) is relevant to understanding both their transport mechanisms and interpreting the in vitro–in vivo extrapolation (IVIVE) required for physiologically-based pharmacokinetic (PBPK) modeling. Here, we use a quantitative western blot method to determine TORs for MATE1 and OCT2 proteins expressed in CHO cells. MATE1 and OCT2, each with a C-terminal V-5 epitope tag, were cell surface biotinylated and the amount of cell surface MATE1 and OCT2 protein was quantified by western analysis, using standard curves for the V5 epitope. Cell surface MATE1 and OCT2 protein represented 25% and 24%, respectively, of the total expression of these proteins in CHO cells. The number of cell surface transporters was ~55 fmol cm−2 for MATE1 and ~510 fmol cm−2 for OCT2. Dividing these values into the different Jmax values for transport of MPP, metformin, and atenolol mediated by MATE1 and OCT2 resulted in calculated TOR values (±SE, n = 4) of 84.0 ± 22.0 s−1 and 2.9 ± 0.6 s−1; metformin, 461.0 ± 121.0 s−1 and 12.6 ± 2.4 s−1; atenolol, 118.0 ± 31.0 s−1, respectively. These values are consistent with the TOR values determined for a variety of exchangers (NHEs), cotransporters (SGLTs, Lac permease), and uniporters (GLUTs, ENTs).

Published

2021

18. Response to Comments on 'Remdesivir and EIDD-1931 Interact with Human Equilibrative Nucleoside Transporters 1 and 2: Implications for Reaching SARS-CoV-2 Viral Sanctuary Sites'

Author

Siennah R. Miller, Meghan E. McGrath, Kimberley M. Zorn, Sean Ekins, Stephen H. Wright, and Nathan J. Cherrington

Subjects

Pharmacology, Alanine, SARS-CoV-2, Molecular Medicine, Humans, Nucleosides, Cytidine, Adenosine Monophosphate, COVID-19 Drug Treatment

Published

2021

19. Genetic evidence that uptake of the fluorescent analog 2NBDG occurs independently of known glucose transporters

Author

Lucas J. D’Souza, Stephen H. Wright, and Deepta Bhattacharya

Subjects

Glucose Transporter Type 1, Glucose, Multidisciplinary, Glucose Transport Proteins, Facilitative, Humans, Biological Transport, Nucleosides, Multiple Myeloma, Fluorescent Dyes

Abstract

The fluorescent derivative of glucose, 2-Deoxy-2-[(7-nitro-2,1,3-benzoxadiazol-4-yl)-amino]-D-glucose (2NBDG), is a widely used surrogate reagent to visualize glucose uptake in live cells at single cell resolution. Using a model of CRISPR-Cas9 gene editing in 5TGM1 myeloma cells, we demonstrate that ablation of the glucose transporter gene Slc2a1 abrogates radioactive glucose uptake but has no effect on the magnitude or kinetics of 2NBDG import. Extracellular 2NBDG, but not NBD-fructose was transported by plasma cells into the cytoplasm suggesting specific activity that is unlinked to glucose import and that of chemically similar compounds. RNA-Seq analysis of primary plasma cells and the 5TGM1 myeloma cell line revealed expression of other candidate glucose transporters. Yet, deletion of these transporters individually or in combination with one another also had no impact on 2NBDG uptake. Ablation of the genes in the Slc29 and Slc35 families of nucleoside and nucleoside sugar transporters as well as the ATP-binding cassette (ABC) transporter family also failed to impact 2NBDG import. Thus, cellular uptake of 2NBDG is promoted by an unknown mechanism and is not a faithful indicator of glucose transport.

Published

2022

20. Nucleoside Reverse Transcriptase Inhibitor Interaction with Human Equilibrative Nucleoside Transporters 1 and 2

Author

Joseph L. Jilek, Raymond K. Hau, Nathan J. Cherrington, Siennah R. Miller, Mark Morales, and Stephen H. Wright

Subjects

Drug Evaluation, Preclinical, Pharmaceutical Science, 030226 pharmacology & pharmacy, Nucleoside Reverse Transcriptase Inhibitor, Equilibrative Nucleoside Transporter 1, 03 medical and health sciences, chemistry.chemical_compound, Zalcitabine, Inhibitory Concentration 50, 0302 clinical medicine, Abacavir, medicine, Humans, Equilibrative-Nucleoside Transporter 2, Blood-Testis Barrier, Uridine transport, Pharmacology, Chemistry, Stavudine, Equilibrative nucleoside transporter, Nucleosides, Articles, Molecular biology, Uridine, 030220 oncology & carcinogenesis, Reverse Transcriptase Inhibitors, Nucleoside, Zidovudine, medicine.drug, HeLa Cells

Abstract

Equilibrative nucleoside transporters (ENTs) transport nucleosides across the blood-testis barrier (BTB). ENTs are of interest to study the disposition of nucleoside reverse-transcriptase inhibitors (NRTIs) in the human male genital tract because of their similarity in structure to nucleosides. HeLa S3 cells express ENT1 and ENT2 and were used to compare relative interactions of these transporters with selected NRTIs. Inhibition of [(3)H]uridine uptake by NBMPR was biphasic, with IC(50) values of 11.3 nM for ENT1 and 9.6 μM for ENT2. Uptake measured with 100 nM NBMPR represented ENT2-mediated transport; subtracting that from total uptake represented ENT1-mediated transport. The kinetics of ENT1- and ENT2-mediated [(3)H]uridine uptake revealed no difference in J(max) (16.53 and 30.40 pmol cm(−2) min(−1)) and an eightfold difference in K(t) (13.6 and 108.9 μM). The resulting fivefold difference in intrinsic clearance (J(max)/K(t)) for ENT1- and ENT2 transport accounted for observed inhibition of [(3)H]uridine uptake by 100 nM NBMPR. Millimolar concentrations of the NRTIs emtricitabine, didanosine, lamivudine, stavudine, tenofovir disoproxil, and zalcitabine had no effect on ENT transport activity, whereas abacavir, entecavir, and zidovudine inhibited both transporters with IC(50) values of ∼200 µM, 2.5 mM, and 2 mM, respectively. Using liquid chromatography-tandem mass spectrometry and [(3)H] compounds, the data suggest that entecavir is an ENT substrate, abacavir is an ENT inhibitor, and zidovudine uptake is carrier-mediated, although not an ENT substrate. These data show that HeLa S3 cells can be used to explore complex transporter selectivity and are an adequate model for studying ENTs present at the BTB. SIGNIFICANCE STATEMENT: This study characterizes an in vitro model using S-[(4-nitrophenyl)methyl]-6-thioinosine to differentiate between equilibrative nucleoside transporter (ENT) 1- and ENT2-mediated uridine transport in HeLa cells. This provides a method to assess the influence of nucleoside reverse-transcriptase inhibitors on natively expressed transporter function. Determining substrate selectivity of the ENTs in HeLa cells can be effectively translated into the activity of these transporters in Sertoli cells that comprise the blood-testis barrier, thereby assisting targeted drug development of compounds capable of circumventing the blood-testis barrier.

Published

2020

21. Molecular and cellular physiology of organic cation transporter 2

Author

Stephen H. Wright

Subjects

0301 basic medicine, Cell physiology, Kidney, Organic cation transport proteins, biology, Physiology, Chemistry, Kinetics, Cationic polymerization, ORGANIC CATION TRANSPORTER 2, Organic Cation Transporter 2, Review, 030226 pharmacology & pharmacy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Biochemistry, Renal physiology, biology.protein, medicine, Animals, Humans

Abstract

Organic cation transporters play a critical role in mediating the distribution of cationic pharmaceuticals. Indeed, organic cation transporter (OCT)2 is the initial step in the renal secretion of organic cations and consequently plays a defining role in establishing the pharmacokinetics of many cationic drugs. Although a hallmark of OCTs is their broad selectivity, this characteristic also makes them targets for unwanted, adverse drug-drug interactions (DDIs), making them a focus for efforts to develop models of ligand interaction that could predict and preempt these adverse interactions. This review discusses the molecular characteristics of these transporters as well as the evidence that established the OCTs as key players in the distribution of organic cations. However, the primary focus is the present understanding of the complexity of ligand interaction with OCTs, particularly OCT2, including evidence for the presence of multiple ligand-binding sites and the influence of substrate structure on the affinity of the transporter for inhibitory ligands. This leads to a discussion of the complexities associated with the development of protocols for assessing the inhibitory potential of new molecular entities to perpetrate unwanted DDIs, the criteria that should be considered in the interpretation of the results of such protocols, and the challenges associated with development of models capable of predicting unwanted DDIs.

Published

2019

22. Kinetic basis of metformin-MPP interactions with organic cation transporter OCT2

Author

Philip J. Sandoval, Stephen H. Wright, Mark Morales, and Timothy W. Secomb

Subjects

0301 basic medicine, Models, Molecular, 1-Methyl-4-phenylpyridinium, endocrine system diseases, Physiology, Protein Conformation, Kinetics, CHO Cells, Binding, Competitive, Models, Biological, 03 medical and health sciences, 0302 clinical medicine, Cricetulus, medicine, Animals, Drug Interactions, Organic cation transport proteins, Binding Sites, biology, Chemistry, ORGANIC CATION TRANSPORTER 2, Cationic polymerization, Organic Cation Transporter 2, Combinatorial chemistry, Metformin, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, biology.protein, Proximal tubule, Selectivity, medicine.drug, Protein Binding, Research Article

Abstract

Organic cation transporter 2 (OCT2) clears the blood of cationic drugs. Efforts to understand OCT2 selectivity as a means to predict the potential of new molecular entities (NMEs) to produce unwanted drug-drug interactions typically assess the influence of the NMEs on inhibition of transport. However, the identity of the substrate used to assess transport activity can influence the quantitative profile of inhibition. Metformin and 1-methyl-4-phenylpyridinium (MPP), in particular, display markedly different inhibitory profiles, with IC50values for inhibition of MPP transport often being more than fivefold greater than IC50values for the inhibition of metformin transport by the same compound, suggesting that interaction of metformin and MPP with OCT2 cannot be restricted to competition for a single binding site. Here, we determined the kinetic basis for the mutual inhibitory interaction of metformin and MPP with OCT2 expressed in Chinese hamster ovary cells. Although metformin did produce simple competitive inhibition of MPP transport, MPP was a mixed-type inhibitor of metformin transport, decreasing the maximum rate of mediated substrate transport and increasing the apparent Michaelis constant ( Ktapp) for OCT2-mediated metformin transport. Furthermore, whereas the IC50value for metformin’s inhibition of MPP transport did not differ from the Ktappvalue for metformin transport, the IC50value for MPP’s inhibition of metformin transport was less than its Ktappvalue for transport. The simplest model to account for these observations required the influence of a distinct inhibitory site for MPP that, when occupied, decreases the translocation of substrate. These observations underscore the complexity of ligand interaction with OCT2 and argue for use of multiple substrates to obtain the needed kinetic assessment of NME interactions with OCT2.

Published

2019

23. Cell Model for Studying Nucleoside Transporters, a Key Component of the Blood‐Testis Barrier

Author

Nathan J. Cherrington, Mark Morales, Stephen H. Wright, Kayla Frost, and Siennah R. Miller

Subjects

Chemistry, Component (UML), Cell model, Genetics, Key (cryptography), Transporter, Molecular Biology, Biochemistry, Nucleoside, Biotechnology, Cell biology, Blood–testis barrier

Published

2019

24. The multidrug transporter MATE1 sequesters OCs within an intracellular compartment that has no influence on OC secretion in renal proximal tubules

Author

William H. Dantzler, Kristen K. Evans, Lucy J. Martinez-Guerrero, and Stephen H. Wright

Subjects

Male, 0301 basic medicine, 1-Methyl-4-phenylpyridinium, Vacuolar Proton-Translocating ATPases, medicine.medical_specialty, Organic Cation Transport Proteins, Physiology, Endosome, ATPase, CHO Cells, Endosomes, Transfection, Kidney Tubules, Proximal, 03 medical and health sciences, chemistry.chemical_compound, Cricetulus, Internal medicine, medicine, Animals, Secretion, Fluorescent Dyes, biology, Vesicle, Chinese hamster ovary cell, Organic Cation Transporter 2, Bafilomycin, Articles, Renal Reabsorption, Molecular biology, Quaternary Ammonium Compounds, Kinetics, Renal Elimination, 4-Chloro-7-nitrobenzofurazan, 030104 developmental biology, Endocrinology, Microscopy, Fluorescence, chemistry, Cytoplasm, biology.protein, Rabbits, Intracellular

Abstract

Secretion of organic cations (OCs) across renal proximal tubules (RPTs) involves basolateral OC transporter (OCT)2-mediated uptake from the blood followed by apical multidrug and toxin extruder (MATE)1/2-mediated efflux into the tubule filtrate. Whereas OCT2 supports electrogenic OC uniport, MATE is an OC/H+exchanger. As assessed by epifluorescence microscopy, cultured Chinese hamster ovary (CHO) cells that stably expressed human MATE1 accumulated the fluorescent OC N, N, N-trimethyl-2-[methyl(7-nitrobenzo[c][l,2,5]oxadiazol-4-yl)amino]ethanaminium (NBD-MTMA) in the cytoplasm and in a smaller, punctate compartment; accumulation in human OCT2-expressing cells was largely restricted to the cytoplasm. A second intracellular compartment was also evident in the multicompartmental kinetics of efflux of the prototypic OC [3H]1-methyl-4-phenylpyridinium (MPP) from MATE1-expressing CHO cells. Punctate accumulation of NBD-MTMA was markedly reduced by coexposure of MATE1-expressing cells with 5 μM bafilomycin (BAF), an inhibitor of V-type H+-ATPase, and accumulation of [3H]MPP and [3H]NBD-MTMA was reduced by >30% by coexposure with 5 μM BAF. BAF had no effect on the initial rate of MATE1-mediated uptake of NBD-MTMA, suggesting that the influence of BAF was a secondary effect involving inhibition of V-type H+-ATPase. The accumulation of [3H]MPP by isolated single nonperfused rabbit RPTs was also reduced >30% by coexposure to 5 μM BAF, suggesting that the native expression in RPTs of MATE protein within endosomes can increase steady-state OC accumulation. However, the rate of [3H]MPP secretion by isolated single perfused rabbit RPTs was not affected by 5 μM BAF, suggesting that vesicles loaded with OCs+are not likely to recycle into the apical plasma membrane at a rate sufficient to provide a parallel pathway for OC secretion.

Published

2016

25. Generation of a hTERT-Immortalized Human Sertoli Cell Model to Study Transporter Dynamics at the Blood-Testis Barrier

Author

Nathan J. Cherrington, Siennah R. Miller, Stephen H. Wright, and Raymond K. Hau

Subjects

sertoli cell, xenobiotic transporter, testes, lcsh:RS1-441, Pharmaceutical Science, Article, lcsh:Pharmacy and materia medica, 03 medical and health sciences, chemistry.chemical_compound, cell immortalization, drug disposition, medicine, blood–testis barrier, Gene, 030304 developmental biology, Blood–testis barrier, 0303 health sciences, 030302 biochemistry & molecular biology, Transporter, Sertoli cell, antiviral, Phenotype, In vitro, Uridine, Cell biology, male contraceptive, medicine.anatomical_structure, chemistry, uridine, nucleoside transport, Nucleoside

Abstract

The blood-testis barrier (BTB) formed by adjacent Sertoli cells (SCs) limits the entry of many chemicals into seminiferous tubules. Differences in rodent and human substrate-transporter selectivity or kinetics can misrepresent conclusions drawn using rodent in vitro models. Therefore, human in vitro models are preferable when studying transporter dynamics at the BTB. This study describes a hTERT-immortalized human SC line (hT-SerC) with significantly increased replication capacity and minor phenotypic alterations compared to primary human SCs. Notably, hT-SerCs retained similar morphology and minimal changes to mRNA expression of several common SC genes, including AR and FSHR. The mRNA expression of most xenobiotic transporters was within the 2-fold difference threshold in RT-qPCR analysis with some exceptions (OAT3, OCT3, OCTN1, OATP3A1, OATP4A1, ENT1, and ENT2). Functional analysis of the equilibrative nucleoside transporters (ENTs) revealed that primary human SCs and hT-SerCs predominantly express ENT1 with minimal ENT2 expression at the plasma membrane. ENT1-mediated uptake of [3H] uridine was linear over 10 min and inhibited by NBMPR with an IC50 value of 1.35 &plusmn, 0.37 nM. These results demonstrate that hT-SerCs can functionally model elements of transport across the human BTB, potentially leading to identification of other transport pathways for xenobiotics, and will guide drug discovery efforts in developing effective BTB-permeable compounds.

Published

2020

26. Determination of hMATE1 Turnover Rate Using Quantitative Western Analysis

Author

Stephen H. Wright and Xiaohong Zhang

Subjects

Animal science, Chemistry, Turnover, Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2020

27. Modeling Blood‐Testis Barrier Characteristics with Novel CRISPR/Cas9 Functional ENT1 and ENT2 Knockout HeLa Cell Lines

Author

Raymond K. Hau, Stephen H. Wright, Nathan J. Cherrington, Erin Q. Jennings, Siennah R. Miller, Xiaohong Rebecca Zhang, and James J. Galligan

Subjects

HeLa, biology, Cell culture, Chemistry, Genetics, CRISPR, biology.organism_classification, Molecular Biology, Biochemistry, Biotechnology, Cell biology, Blood–testis barrier

Published

2020

28. Competitive Counterflow (CCF) To Distinguish Between Transported And Non‐Transported Inhibitors Of MATE1 and MATE2‐K

Author

Stephen H. Wright and Lucy J. Martinez-Guerrero

Subjects

Genetics, Molecular Biology, Biochemistry, Biotechnology

Published

2020

29. Expression and Immunolocalization of Xenobiotic Transporters at the Human Blood‐Testis Barrier

Author

Stephen H. Wright, Nathan J. Cherrington, and Raymond K. Hau

Subjects

Human blood, Xenobiotic transporters, Genetics, Biology, Molecular Biology, Biochemistry, Biotechnology, Cell biology

Published

2020

30. Making Transporter Models for Drug–Drug Interaction Prediction Mobile

Author

Alex M. Clark, Sean Ekins, and Stephen H. Wright

Subjects

Pharmacology, Interaction testing, Computational model, Computer science, Short Communication, Drug-drug interaction, Mobile apps, Membrane Transport Proteins, Pharmaceutical Science, Bayes Theorem, Biological Transport, Transporter, Computational biology, chEMBL, Bioinformatics, Mobile Applications, Models, Biological, Open software, Pharmaceutical Preparations, Profiling (information science), Drug Interactions, Forecasting

Abstract

The past decade has seen increased numbers of studies publishing ligand-based computational models for drug transporters. Although they generally use small experimental data sets, these models can provide insights into structure-activity relationships for the transporter. In addition, such models have helped to identify new compounds as substrates or inhibitors of transporters of interest. We recently proposed that many transporters are promiscuous and may require profiling of new chemical entities against multiple substrates for a specific transporter. Furthermore, it should be noted that virtually all of the published ligand-based transporter models are only accessible to those involved in creating them and, consequently, are rarely shared effectively. One way to surmount this is to make models shareable or more accessible. The development of mobile apps that can access such models is highlighted here. These apps can be used to predict ligand interactions with transporters using Bayesian algorithms. We used recently published transporter data sets (MATE1, MATE2K, OCT2, OCTN2, ASBT, and NTCP) to build preliminary models in a commercial tool and in open software that can deliver the model in a mobile app. In addition, several transporter data sets extracted from the ChEMBL database were used to illustrate how such public data and models can be shared. Predicting drug-drug interactions for various transporters using computational models is potentially within reach of anyone with an iPhone or iPad. Such tools could help prioritize which substrates should be used for in vivo drug-drug interaction testing and enable open sharing of models.

Published

2015

31. Assessment of Substrate-Dependent Ligand Interactions at the Organic Cation Transporter OCT2 Using Six Model Substrates

Author

Kimberley M. Zorn, Stephen H. Wright, Alex M. Clark, Sean Ekins, and Philip J. Sandoval

Subjects

0301 basic medicine, Stereochemistry, Plasma protein binding, CHO Cells, Ligands, Substrate Specificity, 03 medical and health sciences, Cricetulus, In vivo, Cricetinae, Animals, Hypoglycemic Agents, Pharmacology, Organic cation transport proteins, biology, Dose-Response Relationship, Drug, Ligand, Chemistry, Chinese hamster ovary cell, Substrate (chemistry), Organic Cation Transporter 2, Articles, In vitro, Metformin, A-site, 030104 developmental biology, Histamine H2 Antagonists, Models, Chemical, biology.protein, Molecular Medicine, Cimetidine, Protein Binding

Abstract

Organic cation transporter (OCT) 2 mediates the entry step for organic cation secretion by renal proximal tubule cells and is a site of unwanted drug-drug interactions (DDIs). But reliance on decision tree–based predictions of DDIs at OCT2 that depend on IC(50) values can be suspect because they can be influenced by choice of transported substrate; for example, IC(50) values for the inhibition of metformin versus MPP transport can vary by 5- to 10-fold. However, it is not clear whether the substrate dependence of a ligand interaction is common among OCT2 substrates. To address this question, we screened the inhibitory effectiveness of 20 µM concentrations of several hundred compounds against OCT2-mediated uptake of six structurally distinct substrates: MPP, metformin, N,N,N-trimethyl-2-[methyl(7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)amino]ethanaminium (NBD-MTMA), TEA, cimetidine, and 4–4-dimethylaminostyryl-N-methylpyridinium (ASP). Of these, MPP transport was least sensitive to inhibition. IC(50) values for 20 structurally diverse compounds confirmed this profile, with IC(50) values for MPP averaging 6-fold larger than those for the other substrates. Bayesian machine-learning models of ligand-induced inhibition displayed generally good statistics after cross-validation and external testing. Applying our ASP model to a previously published large-scale screening study for inhibition of OCT2-mediated ASP transport resulted in comparable statistics, with approximately 75% of “active” inhibitors predicted correctly. The differential sensitivity of MPP transport to inhibition suggests that multiple ligands can interact simultaneously with OCT2 and supports the recommendation that MPP not be used as a test substrate for OCT2 screening. Instead, metformin appears to be a comparatively representative OCT2 substrate for both in vitro and in vivo (clinical) use.

Published

2017

32. Correlation between Apparent Substrate Affinity and OCT2 Transport Turnover

Author

Philip J. Sandoval, Alyscia Cory Severance, and Stephen H. Wright

Subjects

0301 basic medicine, Organic Cation Transport Proteins, Kinetics, Biological Transport, Active, CHO Cells, 030226 pharmacology & pharmacy, Michaelis–Menten kinetics, Dissociation (chemistry), Metabolism, Transport, and Pharmacogenomics, Substrate Specificity, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cricetulus, Pharmacokinetics, Cations, Cricetinae, Choline, Animals, Humans, Solute Carrier Family 22 Member 5, Pharmacology, Chemistry, Chinese hamster ovary cell, Transporter, 030104 developmental biology, Biochemistry, Pharmaceutical Preparations, Renal physiology, Molecular Medicine

Abstract

Organic cation (OC) transporter 2 (OCT2) mediates the first step in the renal secretion of many cationic drugs: basolateral uptake from blood into proximal tubule cells. The impact of this process on the pharmacokinetics of drug clearance as estimated using a physiologically-based pharmacokinetic approach relies on an accurate understanding of the kinetics of transport because the ratio of the maximal rate of transport to the Michaelis constant (i.e., Jmax/ Kt) provides an estimate of the intrinsic clearance (Clint) used in in vitro–in vivo extrapolation of experimentally determined transport data. Although the multispecificity of renal OC secretion, including that of the OCT2 transporter, is widely acknowledged, the possible relationship between relative affinity of the transporter for its diverse substrates and the maximal rates of their transport has received little attention. In this study, we determined the Jmax and apparent Michaelis constant (Ktapp) values for six structurally distinct OCT2 substrates and found a strong correlation between Jmax and Ktapp; high-affinity substrates [Ktapp values 200 µM, including choline and metformin). Similarly, preloading OCT2-expressing cells with low-affinity substrates resulted in systematically larger trans-stimulated rates of MPP uptake than did preloading with high-affinity substrates. The data are quantitatively consistent with the hypothesis that dissociation of bound substrate from the transporter is rate limiting in establishing maximal rates of OCT2-mediated transport. This systematic relationship may provide a means to estimate Clint for drugs for which transport data are lacking.

Published

2017

33. Xenobiotic transporter expression along the male genital tract

Author

David M. Klein, Nathan J. Cherrington, and Stephen H. Wright

Subjects

Male, medicine.medical_specialty, Genitalia, Male, Biology, Kidney, Toxicology, Article, Xenobiotics, Rats, Sprague-Dawley, chemistry.chemical_compound, Prostate, Internal medicine, medicine, Animals, RNA, Messenger, Vas deferens, Membrane Transport Proteins, Biological Transport, Transporter, Epididymis, Sperm, medicine.anatomical_structure, Endocrinology, Liver, chemistry, Efflux, Xenobiotic

Abstract

The male genital tract plays an important role in protecting sperm by forming a distinct compartment separate from the body which limits exposure to potentially toxic substrates. Transporters along this tract can influence the distribution of xenobiotics into the male genital tract through efflux back into the blood or facilitating the accumulation of toxicants. The aim of this study was to quantitatively determine the constitutive mRNA expression of 30 xenobiotic transporters in caput and cauda regions of the epididymis, vas deferens, prostate, and seminal vesicles from adult Sprague-Dawley rats. The epididymis was found to express at least moderate levels of 18 transporters, vas deferens 15, seminal vesicles 23, and prostate 18. Constitutive expression of these xenobiotic transporters in the male genital tract may provide insight into the xenobiotics that can potentially be transported into these tissues and may provide the molecular mechanism for site specific toxicity of select agents.

Published

2014

34. Localization of Multidrug Resistance-Associated Proteins along the Blood-Testis Barrier in Rat, Macaque, and Human Testis

Author

Nathan J. Cherrington, David M. Klein, and Stephen H. Wright

Subjects

Male, medicine.medical_specialty, Pharmaceutical Science, Rats, Sprague-Dawley, Cell membrane, Internal medicine, Testis, medicine, Animals, Humans, Blood-Testis Barrier, Blood–testis barrier, Epithelial polarity, Pharmacology, biology, Membrane transport protein, Cell Membrane, Membrane Transport Proteins, Articles, Apical membrane, Sertoli cell, Subcellular localization, Immunohistochemistry, Rats, Cell biology, Endocrinology, medicine.anatomical_structure, biology.protein, Macaca, Multidrug Resistance-Associated Proteins

Abstract

The blood-testis barrier (BTB) prevents the entry of many drugs into seminiferous tubules, which can be beneficial for therapy not intended for the testis but may decrease drug efficacy for medications requiring entry to the testis. Previous data have shown that some of the transporters in the multidrug resistance-associated protein (MRP) family (ABCC) are expressed in the testis. By determining the subcellular localization of these transporters, their physiologic function and effect on drug disposition may be better predicted. Using immunohistochemistry (IHC), we determined the site of expression of the MRP transporters expressed in the testis, namely, MRP1, MRP4, MRP5, and MRP8, from immature and mature rats, rhesus macaques, and adult humans. We determined that in all species MRP1 was restricted to the basolateral membrane of Sertoli cells, MRP5 is located in Leydig cells, and MRP8 is located in round spermatids, whereas MRP4 showed species-specific localization. MRP4 is expressed on the basolateral membrane of Sertoli cells in human and nonhuman primates, but on the apical membrane of Sertoli cells in immature and mature rats, representing a potential caution when using rat models as a means for studying drug disposition across the BTB. These data suggest that MRP1 may limit drug disposition into seminiferous tubules, as may MRP4 in human and nonhuman primates but not in rats. These data also suggest that MRP5 and MRP8 may not have a major impact on the penetration of drugs across the BTB.

Published

2013

35. Substrate-Dependent Inhibition of Human MATE1 by Cationic Ionic Liquids

Author

Stephen H. Wright and Lucy J. Martinez-Guerrero

Subjects

1-Methyl-4-phenylpyridinium, Organic Cation Transport Proteins, Stereochemistry, Biological Transport, Active, Ionic Liquids, Pyridinium Compounds, CHO Cells, Binding, Competitive, Metabolism, Transport, and Pharmacogenomics, chemistry.chemical_compound, Cricetulus, Cations, Cricetinae, Animals, Humans, Binding site, Pharmacology, Organic cation transport proteins, biology, Chinese hamster ovary cell, Cationic polymerization, Substrate (chemistry), Transporter, Quaternary Ammonium Compounds, Kinetics, 4-Chloro-7-nitrobenzofurazan, chemistry, Ionic liquid, biology.protein, Molecular Medicine, Pyridinium, Algorithms

Abstract

The multidrug and toxin extruders 1- and 2-K (MATE1 and MATE2-K) are expressed in the luminal membrane of renal proximal tubule cells and provide the active step in the secretion of molecules that carry a net positive charge at physiologic pH, so-called organic cations. The present study tested whether structurally distinct MATE substrates can display different quantitative profiles of inhibition when interacting with structurally distinct ligands. The tested ligands were three structurally similar cationic ionic liquids (ILs, salts in the liquid state: N-butylpyridinium, NBuPy; 1-methyl-3-butylimidazolium, Bmim; and N-butyl-N-methylpyrrolidinium, BmPy). Uptake was measured using Chinese hamster ovary cells that stably expressed MATE1 or MATE2-K. By trans-stimulation, all three ILs were transported by both MATE transporters. The three ILs also inhibited uptake of three structurally distinct MATE substrates: 1-methyl-4-phenylpyridinium (MPP), triethylmethylammonium (TEMA), and N,N,N-trimethyl-2-[methyl(7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)amino]ethanaminium (NBD-MTMA). MATE1 displayed a higher affinity for the pyridinium-based NBuPy (IC50 values, 2–4 µM) than for either the pyrrolidinium- (BmPy; 20–70 µM) or imidazolium-based ILs (Bmim; 15–60 µM). Inhibition of MPP, TEMA, and NBD-MTMA transport by NBuPy was competitive, with comparable Ki values against all substrates. Bmim also competitively blocked the three substrates but with Ki values that differed significantly (20 µM against MPP and 30 µM against NBD-MTMA versus 60 µM against TEMA). Together, these data indicate that renal secretion of ILs by the human kidney involves MATE transporters and suggest that the mechanism of transport inhibition is ligand-dependent, supporting the hypothesis that the binding of substrates to MATE transporters involves interaction with a binding surface with multiple binding sites.

Published

2013

36. Substrate-Dependent Ligand Inhibition of the Human Organic Cation Transporter OCT2

Author

Matthew Belzer, Bhumasamudram Jagadish, Mark Morales, Stephen H. Wright, and Eugene A. Mash

Subjects

1-Methyl-4-phenylpyridinium, Organic Cation Transport Proteins, Stereochemistry, CHO Cells, Ligands, Metabolism, Transport, and Pharmacogenomics, Cricetulus, Cations, Cricetinae, Animals, Humans, IC50, Fluorescent Dyes, Epithelial polarity, Pharmacology, Organic cation transport proteins, biology, Chemistry, Organic Cation Transporter 2, Substrate (chemistry), Biological Transport, 4-Chloro-7-nitrobenzofurazan, Ligand (biochemistry), Metformin, Quaternary Ammonium Compounds, HEK293 Cells, Renal physiology, biology.protein, Molecular Medicine, Selectivity

Abstract

Organic cation transporter 2 (OCT2) mediates the initial step in renal secretion of organic cations: uptake from the blood, across the basolateral membrane, and into the renal proximal tubule cells. Because of its potential as a target for unwanted drug-drug interactions (DDIs), considerable attention has been directed toward understanding the basis of OCT2 selectivity. These studies typically assess selectivity based on ligand inhibition profiles for OCT2-mediated transport of a probe substrate. However, little attention has been given to the potential influence of the substrate on the profile of ligand inhibition. Here we compared the IC50 values obtained for a set of structurally distinct inhibitors against OCT2-mediated transport of three structurally distinct substrates: 1-methyl-4-phenylpyridinium (MPP); metformin; and a novel fluorescent substrate, N,N,N-trimethyl-2-[methyl(7-nitrobenzo[c][l,2,5]oxadiazol-4-yl)amino]ethanaminium iodide (NBD-MTMA). The median IC50 value for inhibition of MPP transport was 9-fold higher than that for inhibition of metformin transport. Similarly, the median IC50 value for inhibition of MPP transport was 5-fold higher than that for NBD-MTMA transport. However, this was not a systematic difference in inhibitory efficacy; the ratio of IC50 values, MPP versus NBD-MTMA, ranged from 88-fold (ipratropium) to 0.3-fold (metformin). These data show that 1) the choice of OCT2 substrate significantly influences both quantitative and qualitative inhibitory interactions with cationic drugs; and 2) ligand interactions with OCT2 are not restricted to competition for a common ligand binding site, consistent with a binding surface characterized by multiple, possibly overlapping interaction sites. Development of predictive models of DDIs with OCT2 must take into account the substrate dependence of ligand interaction with this protein.

Published

2013

37. Multiple mechanisms of ligand interaction with the human organic cation transporter, OCT2

Author

Jaclyn N. Harper and Stephen H. Wright

Subjects

1-Methyl-4-phenylpyridinium, Organic Cation Transport Proteins, Physiology, Kinetics, Carbazoles, CHO Cells, Ligands, Propanolamines, Inhibitory Concentration 50, chemistry.chemical_compound, Cricetulus, Piperidines, Cricetinae, Animals, Humans, Secretion, Benzhydryl Compounds, Tetraethylammonium, Organic cation transport proteins, biology, Ligand, Chinese hamster ovary cell, Organic Cation Transporter 2, Articles, biology.organism_classification, Metformin, chemistry, Biochemistry, biology.protein, Androstenes, Carvedilol, Cimetidine

Abstract

OCT2 is the entry step for organic cation (OC) secretion by renal proximal tubules. Although many drugs inhibit OCT2 activity, neither the mechanistic basis of their inhibition nor their transport status is generally known. Using representatives of several structural classes of OCT2-inhibitory ligands described recently (Kido Y, Matsson P, Giacomini KM. J Med Chem 54: 4548–4558, 2011), we determined the kinetic basis of their inhibition of 1-methyl-4-phenylpyridinium (MPP) transport into Chinese hamster ovary cells that stably expressed hOCT2. The “cluster II” inhibitors (which contain known OCT2 substrates) metformin and cimetidine interacted competitively with MPP. However, other cluster II compounds, including tetraethylammonium (TEA), diphenidol and phenyltoloxamine, were mixed-type inhibitors of MPP transport (i.e., decreasing Jmaxand increasing Kt). A cluster III (neutral steroid) representative, adrenosterone, and a cluster I (large, flexible cation) representative, carvedilol, displayed noncompetitive inhibitory profiles. Competitive counterflow (CCF) was used to determine whether the inhibitory ligands served as substrates of hOCT2. Carvedilol (cluster I) and adrenosterone (cluster III) did not support CCF, consistent with the prediction that members of these structural classes are likely to be nontransported inhibitors of OCT2. The cluster II representatives MPP, metformin, cimetidine, and TEA all supported CCF, consistent with independent assessments of their OCT2-mediated transport. However, the other cluster II representatives, diphenidol and phenyltoloxamine, failed to support CCF, suggesting that neither compound is transported by OCT2. An independent assessment of diphenidol transport (using liquid chromatography with tandem mass spectroscopy) confirmed this observation. The results underscore the caution required for development of predictive models of ligand interaction with multidrug transporters.

Published

2013

38. Lack of Influence of Substrate on Ligand Interaction with the Human Multidrug and Toxin Extruder, MATE1

Author

Sean Ekins, Lucy J. Martinez-Guerrero, Stephen H. Wright, and Mark H Morales

Subjects

0301 basic medicine, Models, Molecular, Time Factors, Organic Cation Transport Proteins, Stereochemistry, CHO Cells, Ligands, Substrate Specificity, Machine Learning, 03 medical and health sciences, Inhibitory Concentration 50, Cricetulus, Cricetinae, Animals, Humans, IC50, Pharmacology, Organic cation transport proteins, biology, Chemistry, Chinese hamster ovary cell, Cationic polymerization, Substrate (chemistry), Bayes Theorem, Biological Transport, Articles, biology.organism_classification, Ligand (biochemistry), Kinetics, 030104 developmental biology, Biochemistry, biology.protein, Molecular Medicine, Pharmacophore

Abstract

Multidrug and toxin extruder (MATE) 1 plays a central role in mediating renal secretion of organic cations, a structurally diverse collection of compounds that includes ∼40% of prescribed drugs. Because inhibition of transport activity of other multidrug transporters, including the organic cation transporter (OCT) 2, is influenced by the structure of the transported substrate, the present study screened over 400 drugs as inhibitors of the MATE1-mediated transport of four structurally distinct organic cation substrates: the commonly used drugs: 1) metformin and 2) cimetidine; and two prototypic cationic substrates, 3) 1-methyl-4-phenylpyridinium (MPP), and 4) the novel fluorescent probe, N,N,N-trimethyl-2-[methyl(7-nitrobenzo[c][1,2,5]oxadiazol-4-yl)amino]ethanaminium iodide. Transport was measured in Chinese hamster ovary cells that stably expressed the human ortholog of MATE1. Comparison of the resulting inhibition profiles revealed no systematic influence of substrate structure on inhibitory efficacy. Similarly, IC50 values for 26 structurally diverse compounds revealed no significant influence of substrate structure on the kinetic interaction of inhibitor with MATE1. The IC50 data were used to generate three-dimensional quantitative pharmacophores that identified hydrophobic regions, H-bond acceptor sites, and an ionizable (cationic) feature as key determinants for ligand binding to MATE1. In summary, in contrast to the behavior observed with some other multidrug transporters, including OCT2, the results suggest that substrate identity exerts comparatively little influence on ligand interaction with MATE1.

Published

2016

39. Computational Modeling to Accelerate the Identification of Substrates and Inhibitors for Transporters That Affect Drug Disposition

Author

Peter W. Swaan, Sean Ekins, James E. Polli, and Stephen H. Wright

Subjects

Drug, Drug-Related Side Effects and Adverse Reactions, media_common.quotation_subject, Computational biology, Biology, Pharmacology, Ligands, Models, Biological, Article, Structure-Activity Relationship, Humans, Drug Interactions, Pharmacology (medical), Repurposing, media_common, Computational model, Drug disposition, Membrane transport protein, Computational Biology, Membrane Transport Proteins, Transporter, Pharmaceutical Preparations, biology.protein, Identification (biology), Efflux

Abstract

We have seen the increased use of computational approaches to predict drug interactions with human transporters that affect drug disposition and may lead to toxicity. These predominantly ligand-based methods use limited experimental data but provide new insights into structure activity relationships (SARs). The promiscuity of ligand interaction with transporters represents a challenge to computational methods. Development of models capable of identifying new transport substrates and unwanted drug-drug interactions requires novel applications of current computational methods. The clinical importance of efflux and uptake transporters in drug disposition is widely acknowledged [1–5] and membrane transporter anomalies are the basis for certain clinical disorders. Consequently, increasing attention is being paid to the potential for transport-based toxicity in vivo, and to unwanted drug-drug interactions [6–9] and consequences from polymorphic transport activity [10]. Furthermore, with hundreds of transporters yet to be characterized, the potential exists for many new drug targets to be discovered [8]. Computational models could therefore enable repurposing of already approved drugs [11] as well as predict the potential for, and ultimately preempt undesirable effects [12–14] that are based on drug-transporter interactions.

Published

2012

40. Twelve Transmembrane Helices Form the Functional Core of Mammalian MATE1 (Multidrug and Toxin Extruder 1) Protein

Author

Xiaohong Zhang, Geoffrey Chang, Florence Tama, Stephen H. Wright, Joseph L. Baker, and Xiao He

Subjects

Male, Models, Molecular, Organic Cation Transport Proteins, CHO Cells, Biology, urologic and male genital diseases, Biochemistry, Antiporters, Protein Structure, Secondary, Cell membrane, Mice, Cricetulus, Bacterial Proteins, Cricetinae, Membrane Biology, Extracellular, medicine, Animals, Humans, Homology modeling, Vibrio cholerae, Molecular Biology, C-terminus, Cell Membrane, Cell Biology, Membrane transport, Transport protein, Protein Transport, Transmembrane domain, medicine.anatomical_structure, Membrane protein, Structural Homology, Protein, Biophysics, Rabbits

Abstract

The x-ray structure of the prototypic MATE family member, NorM from Vibrio cholerae, reveals a protein fold composed of 12 transmembrane helices (TMHs), confirming hydropathy analyses of the majority of (prokaryotic and plant) MATE transporters. However, the mammalian MATEs are generally predicted to have a 13(th) TMH and an extracellular C terminus. Here we affirm this prediction, showing that the C termini of epitope-tagged, full-length human, rabbit, and mouse MATE1 were accessible to antibodies from the extracellular face of the membrane. Truncation of these proteins at or near the predicted junction between the 13(th) TMH and the long cytoplasmic loop that precedes it resulted in proteins that (i) trafficked to the membrane and (ii) interacted with antibodies only after permeabilization of the plasma membrane. CHO cells expressing rbMate1 truncated at residue Gly-545 supported levels of pH-sensitive transport similar to that of cells expressing the full-length protein. Although the high transport rate of the Gly-545 truncation mutant was associated with higher levels of membrane expression (than full-length MATE1), suggesting the 13(th) TMH may influence substrate translocation, the selectivity profile of the mutant indicated that TMH13 has little impact on ligand binding. We conclude that the functional core of MATE1 consists of 12 (not 13) TMHs. Therefore, we used the x-ray structure of NorM to develop a homology model of the first 12 TMHs of MATE1. The model proved to be stable in molecular dynamic simulations and agreed with topology evident from preliminary cysteine scanning of intracellular versus extracellular loops.

Published

2012

41. Simulations of substrate transport in the multidrug transporter EmrD

Author

Florence Tama, Stephen H. Wright, and Joseph L. Baker

Subjects

Carbonyl Cyanide m-Chlorophenyl Hydrazone, Lipid Bilayers, Molecular Dynamics Simulation, Carbonyl cyanide m-chlorophenyl hydrazone, Models, Biological, Biochemistry, Transport Pathway, Article, chemistry.chemical_compound, Structural Biology, Lipid bilayer, Molecular Biology, biology, Membrane transport protein, Escherichia coli Proteins, Membrane Transport Proteins, Transporter, Periplasmic space, Drug Resistance, Multiple, Major facilitator superfamily, chemistry, Periplasm, biology.protein, Biophysics, Efflux

Abstract

EmrD is a multidrug resistance (MDR) transporter from Escherichia coli, which is involved in the efflux of amphipathic compounds from the cytoplasm, and the first MDR member of the major facilitator superfamily (MFS) to be crystallized. Molecular dynamics simulation of EmrD in a phospholipid bilayer was used to characterize the conformational dynamics of the protein. Motions that support a previously proposed lateral diffusion pathway for substrate from the cytoplasmic membrane leaflet into the EmrD central cavity were observed. Additionally, the translocation pathway of metachloro carbonylcyanide phenylhydrazone (CCCP) was probed using both standard and steered molecular dynamics simulation. In particular, interactions of a few specific residues with CCCP have been identified. Finally, a large motion of two residues, Val 45 and Leu 233, was observed with the passage of CCCP into the periplasmic space, placing a lower bound on the extent of opening required at this end of the protein for substrate transport. Overall, our simulations probe details of the transport pathway, motions of EmrD at an atomic level of detail, and offer new insights into the functioning of MDR transporters.

Published

2012

42. Molecular Determinants of Ligand Selectivity for the Human Multidrug and Toxin Extruder Proteins MATE1 and MATE2-K

Author

Bethzaida Astorga, Stephen H. Wright, Sean Ekins, and Mark Morales

Subjects

1-Methyl-4-phenylpyridinium, Organic Cation Transport Proteins, Stereochemistry, Cell Culture Techniques, Gene Expression, CHO Cells, Ligands, Transfection, Polar surface area, Cricetulus, Cricetinae, Molecular descriptor, Animals, Humans, Computer Simulation, Toxins, Biological, Pharmacology, Organic cation transport proteins, biology, Hydrogen bond, Chemistry, Chinese hamster ovary cell, Bayes Theorem, Biological Transport, Ligand (biochemistry), Transport protein, biology.protein, Molecular Medicine, Pharmacophore, Gastrointestinal, Hepatic, Pulmonary, and Renal

Abstract

The present study compared the selectivity of two homologous transport proteins, multidrug and toxin extruders 1 and 2-K (MATE1 and MATE2-K), and developed three-dimensional pharmacophores for inhibitory ligand interaction with human MATE1 (hMATE1). The human orthologs of MATE1 and MATE2-K were stably expressed in Chinese hamster ovary cells, and transport function was determined by measuring uptake of the prototypic organic cation (OC) substrate 1-methyl-4-phenylpyridinium (MPP). Both MATEs had similar apparent affinities for MPP, with K(tapp) values of 4.4 and 3.7 μM for MATE1 and MATE2-K, respectively. Selectivity was assessed for both transporters from IC(50) values for 59 structurally diverse compounds. Whereas the two transporters discriminated markedly between a few of the test compounds, the IC(50) values for MATE1 and MATE2-K were within a factor of 3 for most of them. For hMATE1 there was little or no correlation between IC(50) values and the individual molecular descriptors LogP, total polar surface area, or pK(a). The IC(50) values were used to generate a common-features pharmacophore, quantitative pharmacophores for hMATE1, and a bayesian model suggesting molecular features favoring and not favoring the interaction of ligands with hMATE1. The models identified hydrophobic regions, hydrogen bond donor and hydrogen bond acceptor sites, and an ionizable (cationic) feature as key determinants for ligand binding to MATE1. In summary, using a combined in vitro and computational approach, MATE1 and MATE2-K were found to have markedly overlapping selectivities for a broad range of cationic compounds, including representatives from seven novel drug classes of Food and Drug Administration-approved drugs.

Published

2012

43. Differences in the substrate binding regions of renal organic anion transporters 1 (OAT1) and 3 (OAT3)

Author

Mark Morales, Stephen H. Wright, Ryan M. Pelis, Bethzaida Astorga, and Theresa M. Wunz

Subjects

Organic anion transporter 1, Physiology, Stereochemistry, Organic Anion Transport Protein 1, CHO Cells, Organic Anion Transporters, Sodium-Independent, Structure-Activity Relationship, Cricetulus, Cricetinae, Animals, Humans, Binding site, Chelating Agents, chemistry.chemical_classification, Alanine, Binding Sites, biology, Substrate (chemistry), Unithiol, Articles, chemistry, Biochemistry, Structural Homology, Protein, biology.protein, Thiol, Cysteine, Organic anion

Abstract

This study examined the selectivity of organic anion transporters OAT1 and OAT3 for structural congeners of the heavy metal chelator 2,3-dimercapto-1-propanesulfonic acid (DMPS). Thiol-reactive reagents were also used to test structural predictions based on a homology model of OAT1 structure. DMPS was near equipotent in its ability to inhibit OAT1 (IC50 = 83 μM) and OAT3 (IC50 = 40 μM) expressed in Chinese hamster ovary cells. However, removal of a thiol group (3-mercapto-1-propanesulfonic acid) resulted in a 2.5-fold increase in IC50 toward OAT1 vs. a ∼55-fold increase in IC50 toward OAT3. The data suggested that compound volume/size is important for binding to OAT1/OAT3. The sensitivity to HgCl2 of OAT1 and OAT3 was also dramatically different, with IC50 values of 104 and 659 μM, respectively. Consistent with cysteines of OAT1 being more accessible from the external medium than those of OAT3, thiol-reactive reagents reacted preferentially with OAT1 in cell surface biotinylation assays. OAT1 was less sensitive to HgCl2 inhibition and less reactive toward membrane-impermeant thiol reactive reagents following mutation of cysteine 440 (C440) to an alanine. These data indicate that C440 in transmembrane helix 10 of OAT1 is accessible from the extracellular space. Indeed, C440 was exposed to the aqueous phase of the presumptive substrate translocation pathway in a homology model of OAT1 structure. The limited thiol reactivity in OAT3 suggests that the homologous cysteine residue (C428) is less accessible. Consistent with their homolog-specific selectivities, these data highlight structural differences in the substrate binding regions of OAT1 and OAT3.

Published

2011

44. Characterization of the Inhibitory Effects ofN-Butylpyridinium Chloride and Structurally Related Ionic Liquids on Organic Cation Transporters 1/2 and Human Toxic Extrusion Transporters 1/2-K In Vitro and In Vivo

Author

Yaofeng Cheng, I. Glenn Sipes, Lucy J. Martinez-Guerrero, R. K. Kuester, Stephen H. Wright, and Michelle J. Hooth

Subjects

Male, Organic Cation Transport Proteins, Pyridinium Compounds, Stereochemistry, Ionic Liquids, Pharmaceutical Science, CHO Cells, Chloride, chemistry.chemical_compound, Cricetulus, In vivo, Cricetinae, medicine, Animals, Humans, Pharmacology, Organic cation transport proteins, biology, Organic Cation Transporter 2, Transporter, Articles, Metformin, Rats, Inbred F344, In vitro, Rats, chemistry, Ionic liquid, biology.protein, Catecholamine Plasma Membrane Transport Proteins, Pyridinium, medicine.drug

Abstract

Ionic liquids (ILs) are a class of salts that are expected to be used as a new source of solvents and for many other applications. Our previous studies revealed that selected ILs, structurally related organic cations, are eliminated exclusively in urine as the parent compound, partially mediated by renal transporters. This study investigated the inhibitory effects of N-butylpyridinium chloride (NBuPy-Cl) and structurally related ILs on organic cation transporters (OCTs) and multidrug and toxic extrusion transporters (MATEs) in vitro and in vivo. After Chinese hamster ovary cells expressing rat (r) OCT1, rOCT2, human (h) OCT2, hMATE1, or hMATE2-K were constructed, the ability of NBuPy-Cl, 1-methyl-3-butylimidazolium chloride (Bmim-Cl), N-butyl-N-methylpyrrolidinium chloride (BmPy-Cl), and alkyl substituted pyridinium ILs to inhibit these transporters was determined in vitro. NBuPy-Cl (0, 0.5, or 2 mg/kg per hour) was also infused into rats to assess its effect on the pharmacokinetics of metformin, a substrate of OCTs and MATEs. NBuPy-Cl, Bmim-Cl, and BmPy-Cl displayed strong inhibitory effects on these transporters (IC(50) = 0.2-8.5 μM). In addition, the inhibitory effects of alkyl-substituted pyridinium ILs on OCTs increased dramatically as the length of the alkyl chain increased. The IC(50) values were 0.1, 3.8, 14, and 671 μM (hexyl-, butyl-, and ethyl-pyridinium and pyridinium chloride) for rOCT2-mediated metformin transport. Similar structurally related inhibitory kinetics were also observed for rOCT1 and hOCT2. The in vivo coadministration study revealed that NBuPy-Cl reduced the renal clearance of metformin in rats. These results demonstrate that ILs compete with other substrates of OCTs and MATEs and could alter the in vivo pharmacokinetics of such substrates.

Published

2011

45. Solution Structure of the Leader Sequence of the Patellamide Precursor Peptide, PatE1-34

Author

Stephen H. Wright, Gary S. Thompson, Marcel Jaspars, Wael E. Houssen, Arnout P. Kalverda, and Sharon M. Kelly

Subjects

Circular dichroism, Magnetic Resonance Spectroscopy, Molecular Sequence Data, Peptide, Sequence alignment, Sequence (biology), Molecular Dynamics Simulation, Protein Sorting Signals, Biology, Biochemistry, Protein Structure, Secondary, chemistry.chemical_compound, Bacterial Proteins, Biosynthesis, Amino Acid Sequence, Protein Precursors, Molecular Biology, Peptide sequence, Protein secondary structure, chemistry.chemical_classification, Sequence Homology, Amino Acid, Circular Dichroism, Organic Chemistry, Hydrogen-Ion Concentration, Combinatorial chemistry, chemistry, Prochloron, Helix, Molecular Medicine, Peptides, Sequence Alignment

Abstract

The solution structure of the leader sequence of the patellamide precursor peptide was analysed by using CD and determined with NOE-restrained molecular dynamics calculations. This leader sequence is highly conserved in the precursor peptides of some other cyanobactins harbouring heterocycles, and is assumed to play a role in targeting the precursor peptide to the post-translational machinery. The sequence was observed to form an alpha-helix spanning residues 13-28 with a hydrophobic surface on one side of the helix. This hydrophobic surface is proposed to be the site of the initial binding with modifying enzymes.

Published

2010

46. Organic anion transporter 3 (OAT3) and renal transport of the metal chelator 2,3-dimercapto-1-propanesulfonic acid (DMPS)

Author

Bernhard Ugele, Gerhard Burckhardt, Andrew Bahn, Stephen H. Wright, Nikolaus Gersdorff, Matthias Rödiger, and Xiaohong ZhangX. Zhang

Subjects

Organic anion transporter 1, Physiology, 2,3-Dimercapto-1-propanesulfonic acid, Organic Anion Transporters, Sodium-Independent, Metal Chelator, Article, Cell Line, Nephrotoxicity, Kidney Tubules, Proximal, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Metals, Heavy, Physiology (medical), medicine, Animals, Humans, IC50, Chelating Agents, Fluorescent Dyes, 030304 developmental biology, Pharmacology, 0303 health sciences, Kidney, biology, Unithiol, General Medicine, Transfection, Fluoresceins, 3. Good health, Protein Transport, medicine.anatomical_structure, chemistry, Biochemistry, 030220 oncology & carcinogenesis, biology.protein, Rabbits, Efflux, Oxidation-Reduction

Abstract

Recent investigations involving intact rabbit renal proximal tubules indicated that organic anion transporter 3 (OAT3) may be involved in the transport of 2,3-dimercapto-1-propanesulfonic acid (DMPS). Therefore, we evaluated the interaction of OAT3 with DMPS to determine the effect of OAT3 on basolateral DMPS uptake. We used stably transfected HEK293 cells expressing human and rabbit orthologs of the exchanger OAT1 and OAT3. Using 6-carboxyfluorescein (6-CF) as a substrate, the IC50determinations for reduced DMPS (DMPSH) revealed a stronger interaction with OAT1 than with OAT3 (rbOAT1, 123.3 ± 13.7; hOAT1, 85.1 ± 8.8; rbOAT3, 171.7 ± 22.3; and hOAT3, 172.2 ± 36.4 µmol/L). However, inhibition of 6-CF uptake by the oxidized form of DMPS (DMPSS), the main form of DMPS in the blood, showed a greater affinity for OAT3 (rbOAT1, 237.4 ± 23; hOAT1, 104.6 ± 13.1; rbOAT3, 52.4 ± 7.6; and hOAT3, 31.6 ± 6.6 µmol/L). To determine whether DMPSH and DMPSS are substrates for OAT3, we performed efflux studies with [14C]glutarate and inwardly directed gradients of glutarate. The inhibitors trans-stimulated the efflux of [14C]glutarate, suggesting that OAT3 may be able to transport both forms of DMPS. On the basis of the substantial interaction of OAT3 with DMPSS, we conclude that OAT3 represents the dominant basolateral player in renal detoxification processes resulting from use of DMPS.

Published

2010

47. Renal mate function in the context of drug development

Author

Stephen H. Wright

Subjects

Pharmacology, Cognitive science, Drug development, media_common.quotation_subject, Pharmaceutical Science, Pharmacology (medical), Context (language use), Function (engineering), Psychology, media_common

Published

2018

48. MATE1 has an external COOH terminus, consistent with a 13-helix topology

Author

Xiaohong Zhang and Stephen H. Wright

Subjects

Models, Molecular, 1-Methyl-4-phenylpyridinium, Cell Membrane Permeability, Organic Cation Transport Proteins, Physiology, Stereochemistry, CHO Cells, Transfection, Models, Biological, Protein Structure, Secondary, Cell membrane, Structure-Activity Relationship, Cricetulus, Cytosol, Protein structure, Cricetinae, medicine, Animals, Structure–activity relationship, Cysteine, Organic cation transport proteins, biology, Chemistry, Cell Membrane, Mutagenesis, Biological Transport, Articles, biology.organism_classification, Immunohistochemistry, Recombinant Proteins, Protein Structure, Tertiary, Kinetics, medicine.anatomical_structure, Biochemistry, Helix, Mutagenesis, Site-Directed, biology.protein, Rabbits

Abstract

The mammalian members of the Multidrug And Toxin Extruder family, i.e., MATE1 and MATE2-K, are suspected of mediating the luminal step in renal secretion of organic cations. The 1,000+ prokaryotic/fungal/plant MATE family members are predicted to have 12 transmembrane helices (TMHs), whereas MATE1/2-K appear to have an additional (13th) COOH-terminal helix. Here, we determined whether rabbit MATE1 has an external COOH terminus, consistent with the presence of 13 TMHs. A V5 epitope tag at the COOH terminus of MATE1 was freely accessible to external V5 antibody, whereas tags at the NH2 terminus, or at sites of truncation within the long cytoplasmic loop between predicted TMHs 12 and 13, were only accessible to the V5 antibody following permeabilization of the membrane. The truncated mutants that lacked TMH13 still retained transport activity, indicating that the terminal helix was not necessary for transport function. Cells that expressed a mutant lacking only TMH13 displayed similar Kt and Jmax values to those of the full-length protein, although when normalized to protein expressed at the plasma membrane, the transport rate of the mutant was 2-biotin. Δ13Cys mutants with an added cysteine residue at the truncation sites within the terminal cytoplasmic loop reacted with maleimide biotin only after permeabilization of the membrane, whereas a mutant with a cysteine residue at the COOH terminus was freely accessible to maleimide biotin. These data are consistent with a mammalian MATE topology that includes 13 TMHs and indicate that the terminal TMH, although not necessary for transport function, may influence the turnover characteristics of the transporter.

Published

2009

49. Characterization of the Disposition and Toxicokinetics ofN-Butylpyridinium Chloride in Male F-344 Rats and Female B6C3F1 Mice and Its Transport by Organic Cation Transporter 2

Author

Stephen H. Wright, Michelle J. Hooth, Yaofeng Cheng, and I. G. Sipes

Subjects

Male, medicine.medical_specialty, Organic Cation Transport Proteins, Pharmaceutical Science, Pyridinium Compounds, CHO Cells, Urine, Absorption (skin), Excretion, Mice, Route of administration, Cricetulus, Pharmacokinetics, Oral administration, Cricetinae, Internal medicine, medicine, Animals, Toxicokinetics, Pharmacology, Chemistry, Organic Cation Transporter 2, Articles, Rats, Inbred F344, Rats, Bioavailability, Endocrinology, Female

Abstract

Studies were conducted to characterize the effect of dose and route of administration on the disposition of N-butylpyridinium chloride (NBuPy-Cl), an ionic liquid with solvent properties. Urine was the major route of NBuPy-Cl excretion after intravenous (5 mg/kg), single oral (0.5, 5, or 50 mg/kg), or repeated oral (50 mg/kg/day, 5 days) administration to male F-344 rats and single oral (50 mg/kg) administration to female B6C3F1 mice. Depending on the vehicle, absorption after dermal application (5 mg/kg, 125 μg/cm2) was 10 to 35% at 96 h. After the single intravenous dose, the blood concentration of NBuPy-Cl decreased in a biphasic manner with an elimination half-life of 2.2 h and a clearance of 7 ml/min. After single oral administration of NBuPy-Cl (50 mg/kg), maximum blood concentration was reached at 1.3 h, and the bioavailability was determined to be 47% at 6 h based on the blood toxicokinetics and 67% at 72 h based on urinary excretion. In all the urine and blood samples, only the parent compound was detected. Coadministration of NBuPy-Cl and inulin (by intravenous injection) revealed that the clearance of NBuPy-Cl exceeded the rat glomerular filtration rate. After incubation with Chinese hamster ovary cells expressing human organic cation transporter 2 (hOCT2), NBuPy-Cl was transported effectively (Kt = 18 μM), and also a potent inhibitor of hOCT2 mediated tetraethylammonium transport (IC50 = 2.3 μM). In summary, NBuPy-Cl is partially absorbed from the gastrointestinal tract and eliminated rapidly in the urine as parent compound most likely by renal glomerular filtration and OCT2-mediated secretion.

Published

2009

50. Influence of Estrogen and Xenoestrogens on Basolateral Uptake of Tetraethylammonium by Opossum Kidney Cells in Culture

Author

Carlotta E. Groves, Randall C. Hartman, Ryan M. Pelis, Stephen H. Wright, and Theresa M. Wunz

Subjects

medicine.medical_specialty, Organic Cation Transport Proteins, medicine.drug_class, Diethylstilbestrol, Estrogen receptor, Biology, Kidney, chemistry.chemical_compound, Phenols, Internal medicine, medicine, Animals, RNA, Messenger, Benzhydryl Compounds, Fulvestrant, Cells, Cultured, Pharmacology, Estradiol, Organic Cation Transporter 1, Kidney metabolism, Opossums, Tetraethylammonium Compounds, Xenoestrogen, medicine.anatomical_structure, Endocrinology, chemistry, Estrogen, Molecular Medicine, Estrogen receptor alpha, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

The sex steroid hormone estrogen down-regulates renal organic cation (OC) transport in animals, and it may contribute to sex-related differences in xenobiotic accumulation and excretion. Also, the presence of various endocrine-disrupting chemicals, i.e., environmental chemicals that possess estrogenic activity (e.g., xenoestrogens) may down-regulate various transporters involved in renal accumulation and excretion of xenobiotics. The present study characterizes the mechanism by which long-term (6-day) incubation with physiological concentrations of 17beta-estradiol (E(2)) or the xenoestrogens diethylstilbestrol (DES) and bisphenol A (BPA) regulates the basolateral membrane transport of the OC tetraethylammonium (TEA) in opossum kidney (OK) cell renal cultures. Both 17beta-E(2) and the xenoestrogen DES produced a dose- and time-dependent inhibition of basolateral TEA uptake in OK cell cultures, whereas the weakly estrogenic BPA had no effect on TEA uptake. Treatment for 6 days with either 1 nM 17beta-E(2) or DES reduced TEA uptake by approximately 30 and 40%, respectively. These effects were blocked completely by the estrogen receptor antagonist ICI 182780 (Faslodex, fulvestrant), suggesting that these estrogens regulate OC transport through the estrogen receptor, which was detected (estrogen receptor alpha) in OK cell cultures by reverse transcription-polymerase chain reaction. The J(max) value for TEA uptake in 17beta-E(2)- and DES-treated OK cell cultures was approximately 40 to 50% lower than for ethanol-treated cultures, whereas K(t) was unaffected. This reduction in transport capacity was correlated with a reduction in OC transporter OCT1 protein expression following treatment with both agents.

Published

2007