Molecular Cloning and Functional Characterization of Nitrobenzylthioinosine (NBMPR)-sensitive (es) and NBMPR-insensitive (ei) Equilibrative Nucleoside Transporter Proteins (rENT1 and rENT2) from Rat Tissues

Yao, Sylvia Y. M.; Ng, Amy M. L.; Muzyka, William R.; Griffiths, Mark; Cass, Carol E.; Baldwin, Stephen A.; Young, James D.

doi:10.1074/jbc.272.45.28423

Cited by 216 publications

(273 citation statements)

References 33 publications

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“…9). Treatment with 100 M NBMPR, which inhibits ENT1 and ENT2 (34,52), yielded similar results. Therefore, ENT1 is a major RBV transporter in primary human PBMCs.…”

supporting

confidence: 68%

“…1D). No significant reduction in RBV uptake was observed with a higher concentration of NBMPR (100 M), which inhibits both ENT1 and ENT2 (34,52). While the literature indicates that NBMPR treatment specifically inhibits ENT-mediated transport, we cannot exclude the remote possibility that another NBMPR-sensitive RBV transporter exists (34,52).…”

Section: Rbv R Huh75 Cells With Reduced Rbv Uptakementioning

confidence: 55%

“…No significant reduction in RBV uptake was observed with a higher concentration of NBMPR (100 M), which inhibits both ENT1 and ENT2 (34,52). While the literature indicates that NBMPR treatment specifically inhibits ENT-mediated transport, we cannot exclude the remote possibility that another NBMPR-sensitive RBV transporter exists (34,52). Inhibition of concentrative transport through phloridzin treatment, an inhibitor of sodium-dependent nucleoside transport (25,47), did not reduce RBV uptake in cells, unless they expressed CNT3 via transfection ( Fig.…”

Section: Rbv R Huh75 Cells With Reduced Rbv Uptakementioning

confidence: 99%

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Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Ibarra

Jain

Pfeiffer

2011

J Virol

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Many individuals infected with hepatitis C virus (HCV) develop a chronic infection, and of those who are treated with pegylated interferon and ribavirin (RBV), many do not respond. While the nucleoside analog RBV improves treatment outcome, and will likely be an important component of therapy with next-generation viral inhibitors, RBV's mechanism is controversial. Most of RBV's proposed mechanisms require RBV import into cells. Therefore, we explored whether host-based RBV resistance develops through reduced cellular uptake, akin to chemotherapy resistance in some cancers. We examined the effect of host-based RBV resistance on HCV replication in cultured hepatoma Huh7.5 liver cells and whether RBV resistance develops in HCV patients. When Huh7.5 cells were exposed to RBV, resistance developed through reduced RBV uptake via the ENT1 nucleoside transporter and antiviral efficacy was reduced. The uptake defect in RBV-resistant cells was specific to RBV, since transport of another ENT1 substrate, cytidine, was unaffected. Importantly, RBV uptake significantly declined in HCV patient peripheral blood mononuclear cells (PBMCs) following 4 weeks of therapy. Furthermore, maintenance of RBV uptake correlated with rapid treatment response. Our results uncovered a novel form of antiviral drug resistance and suggest that host-based RBV resistance develops in HCV patients undergoing therapy and that maintenance of RBV uptake may contribute to rapid viral clearance.

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“…9). Treatment with 100 M NBMPR, which inhibits ENT1 and ENT2 (34,52), yielded similar results. Therefore, ENT1 is a major RBV transporter in primary human PBMCs.…”

supporting

confidence: 68%

Section: Rbv R Huh75 Cells With Reduced Rbv Uptakementioning

confidence: 55%

Section: Rbv R Huh75 Cells With Reduced Rbv Uptakementioning

confidence: 99%

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Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Ibarra

Jain

Pfeiffer

2011

J Virol

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“…These types include ENT1, ENT2, ENT3, ENT4, and CNT1, CNT2, CNT3. ENT1 is sensitive to nanomolar concentrations of nitrobenzylthioinosine (nitrobenzylmercaptopurine riboside; NBMPR), whereas ENT2 is resistant to NBMPR up to 1 mM (Baldwin et al, 1999;Yao et al, 1997). Furthermore, ENT1 and ENT2 are widely expressed throughout the central nervous system (Jennings et al, 1998;, while ENT3 appears to be expressed outside the CNS (Baldwin et al, 2005).…”

Section: Adenosine Transportmentioning

confidence: 99%

Adenosine Signaling in Striatal Circuits and Alcohol Use Disorders

Nam

Bruner

Choi

2013

Molecules and Cells

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Adenosine signaling has been implicated in the pathophysiology of alcohol use disorders and other psychiatric disorders such as anxiety and depression. Numerous studies have indicated a role for A1 receptors (A1R) in acute ethanol-induced motor incoordination, while A2A receptors (A2AR) mainly regulate the rewarding effect of ethanol in mice. Recent findings have demonstrated that dampened A2AR-mediated signaling in the dorsomedial striatum (DMS) promotes ethanol-seeking behaviors. Moreover, decreased A2AR function is associated with decreased CREB activity in the DMS, which enhances goal-oriented behaviors and contributes to excessive ethanol drinking in mice. Interestingly, caffeine, the most commonly used psychoactive substance, is known to inhibit both the A1R and A2AR. This dampened adenosine receptor function may mask some of the acute intoxicating effects of ethanol. Furthermore, based on the fact that A2AR activity plays a role in goal-directed behavior, caffeine may also promote ethanol-seeking behavior. The A2AR is enriched in the striatum and exclusively expressed in striatopallidal neurons, which may be responsible for the regulation of inhibitory behavioral control over drug rewarding processes through the indirect pathway of the basal ganglia circuit. Furthermore, the antagonistic interactions between adenosine and dopamine receptors in the striatum also play an integral role in alcoholism and addiction-related disorders. This review focuses on regulation of adenosine signaling in striatal circuits and the possible implication of caffeine in goal-directed behaviors and addiction.

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“…Two ENT and three CNT functional isoforms have been identified. Human (h) and rat (r) ENT1 and ENT2 transport pyrimidine and purine nucleosides and are distinguished functionally by differences in sensitivity to inhibition by nitrobenzylthioinosine (NBMPR) and vasoactive drugs, and by the ability of hENT2 and rENT2 to also transport nucleobases (Griffiths et al, 1997a(Griffiths et al, , 1997bYao et al, 1997;Crawford et al, 1998;Yao et al, 2002a). CNT1 and CNT2 both transport uridine and adenosine, but are otherwise selective for pyrimidine (hCNT1 and rCNT1) and purine (hCNT2 and rCNT2) nucleosides (Huang et al, 1994;Che et al, 1995, Yao et al, 1996aWang et al, 1997;Ritzel et al, 1997Ritzel et al, , 1998.…”

Section: Introductionmentioning

confidence: 99%

Functional characterization of a H⁺/nucleoside co‐transporter (CaCNT) from Candida albicans, a fungal member of the concentrative nucleoside transporter (CNT) family of membrane proteins

Loewen

Mohabir

et al. 2003

Yeast

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Human and other mammalian concentrative (Na + -linked) nucleoside transport proteins belong to a membrane protein family (CNT, TC 2.A.41) that also includes Escherichia coli H + -dependent nucleoside transport protein NupC. Here, we report the cDNA cloning and functional characterization of a CNT family member from the pathogenic yeast Candida albicans. This 608 amino acid residue H + /nucleoside symporter, designated CaCNT, contains 13 predicted transmembrane domains (TMs), but lacks the exofacial, glycosylated carboxyl-terminus of its mammalian counterparts. When produced in Xenopus oocytes, CaCNT exhibited transport activity for adenosine, uridine, inosine and guanosine but not cytidine, thymidine or the nucleobase hypoxanthine. Apparent K m values were in the range 16-64 µM, with V max : K m ratios of 0.58-1.31. CaCNT also accepted purine and uridine analogue nucleoside drugs as permeants, including cordycepin (3 -deoxyadenosine), a nucleoside analogue with anti-fungal activity. Electrophysiological measurements under voltage clamp conditions gave a H + to [ 14 C]uridine coupling ratio of 1 : 1. CaCNT, obtained from logarithmically growing cells, is the first described cationcoupled nucleoside transporter in yeast, and the first member of the CNT family of proteins to be characterized from a unicellular eukaryotic organism.

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Molecular Cloning and Functional Characterization of Nitrobenzylthioinosine (NBMPR)-sensitive (es) and NBMPR-insensitive (ei) Equilibrative Nucleoside Transporter Proteins (rENT1 and rENT2) from Rat Tissues

Cited by 216 publications

References 33 publications

Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Adenosine Signaling in Striatal Circuits and Alcohol Use Disorders

Functional characterization of a H⁺/nucleoside co‐transporter (CaCNT) from Candida albicans, a fungal member of the concentrative nucleoside transporter (CNT) family of membrane proteins

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Molecular Cloning and Functional Characterization of Nitrobenzylthioinosine (NBMPR)-sensitive (es) and NBMPR-insensitive (ei) Equilibrative Nucleoside Transporter Proteins (rENT1 and rENT2) from Rat Tissues

Cited by 216 publications

References 33 publications

Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Host-Based Ribavirin Resistance Influences Hepatitis C Virus Replication and Treatment Response

Adenosine Signaling in Striatal Circuits and Alcohol Use Disorders

Functional characterization of a H+/nucleoside co‐transporter (CaCNT) from Candida albicans, a fungal member of the concentrative nucleoside transporter (CNT) family of membrane proteins

Contact Info

Product

Resources

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Functional characterization of a H⁺/nucleoside co‐transporter (CaCNT) from Candida albicans, a fungal member of the concentrative nucleoside transporter (CNT) family of membrane proteins