Tamoxifen and its active metabolites inhibit dopamine transporter function independently of the estrogen receptors

Mikelman, Sarah; Guptaroy, Bipasha; Gnegy, Margaret E.

doi:10.1111/jnc.13955

Cited by 9 publications

(13 citation statements)

References 16 publications

(16 reference statements)

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“…In a recent study, Mikelman et al show that tamoxifen interacts with the dopamine transporter (DAT) and can block amphetamine‐stimulated dopamine release as well as blocking dopamine reuptake in rat synaptosomes . While acute tamoxifen exposure did not change locomotor behavior, it was effective at blocking the locomotor‐stimulating effects of amphetamine . It is possible that the neonatal DAT stimulation by tamoxifen caused the mild hyperactivity when the mice were tested as adults, though it is also possible that modulation of the estrogen receptor played a role.…”

Section: Discussionmentioning

confidence: 99%

“…36 While acute tamoxifen exposure did not change locomotor behavior, it was effective at blocking the locomotorstimulating effects of amphetamine. 36,37 It is possible that the neonatal DAT stimulation by tamoxifen caused the mild hyperactivity when the mice were tested as adults, though it is also possible that modulation of the estrogen receptor played a role. Together, these data add to the growing literature that behavioral studies employing tamoxifen, especially those looking at dopamine-modulated behaviors, should always include vehicle-treated controls.…”

Section: Discussionmentioning

confidence: 99%

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Deletion of the creatine transporter gene in neonatal, but not adult, mice leads to cognitive deficits

Udobi

Delcimmuto

Kokenge

et al. 2019

J of Inher Metab Disea

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Creatine (Cr) is a guanidino compound that provides readily available phosphate pools for the regeneration of spent adenosine triphosphate (ATP). The lack of brain Cr causes moderate to severe intellectual disability, language impairment, and epilepsy. The most prevalent cause of Cr deficiency are mutations in the X‐linked SLC6A8 (Creatine transporter; CrT) gene, known as CrT deficiency (CTD). One of the most critical areas that need to be addressed is whether Cr is necessary for brain development. To address this concern, the Slc6a8 gene was knocked out in either neonatal (postnatal day (P)5) or adult (P60) mice using a tamoxifen‐inducible Cre recombinase driven by the human ubiquitin C (UBC) promoter. Mice were tested in the Morris water maze, novel, object recognition, and conditioned fear 60 days after Slc6a8 deletion. In addition, overnight locomotor activity was analyzed. Mice that had the gene deleted on P5 showed deficits in the Morris water maze and novel object recognition, while there were no deficits in P60 knockout mice. Interestingly, the P5 knockout mice showed hyperactivity during the dark phase; however, when examining control mice, the effect was due to the administration of tamoxifen from P5 to 10. Taken together, the results of this study show that Cr is necessary during periods of brain development involved in spatial and object learning. This study also highlights the continued importance of using proper control groups for behavioral testing.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Deletion of the creatine transporter gene in neonatal, but not adult, mice leads to cognitive deficits

Udobi

Delcimmuto

Kokenge

et al. 2019

J of Inher Metab Disea

View full text Add to dashboard Cite

show abstract

“…Tamoxifen is a widely prescribed selective estrogen receptor modulator (SERM) used in the treatment and prevention of estrogen receptor-positive breast cancer (Jordan, 2014). It has long been known that the drug tamoxifen affects the dopaminergic system, yet the mechanisms by which it does so have remained unclear (Mikelman et al, 2017). Tamoxifen causes a small but significant increase in extracellular dopamine levels in the nucleus accumbens after peripheral administration (Chaurasia et al, 1998) and also inhibits amphetamine-stimulated hyperactivity (Einat et al, 2007;Cechinel-Recco et al, 2012;Pereira et al, 2014), which relies on elevation of extracellular dopamine levels in the striatum (French, 1986).…”

Section: Introductionmentioning

confidence: 99%

“…The DAT is responsible for clearing dopamine from the extracellular space after its release and in this capacity is a crucial mechanism for regulating dopaminergic signaling (Jaber et al, 1997). Although tamoxifen was shown to block amphetamine-stimulated locomotor behavior (Einat et al, 2007) and we previously demonstrated that it inhibits DAT function independently of its action as an SERM (Mikelman et al, 2017), no studies reported to date have systematically examined the interaction between tamoxifen and the DAT.…”

Section: Introductionmentioning

confidence: 99%

Tamoxifen Directly Interacts with the Dopamine Transporter

Mikelman

Guptaroy

Schmitt

et al. 2018

J Pharmacol Exp Ther

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The selective estrogen receptor modulator tamoxifen increases extracellular dopamine in vivo and acts as a neuroprotectant in models of dopamine neurotoxicity. We investigated the effect of tamoxifen on dopamine transporter (DAT)-mediated dopamine uptake, dopamine efflux, and [H]WIN 35,428 [(-)-2--carbomethoxy-3--(4-fluorophenyl)tropane] binding in rat striatal tissue. Tamoxifen dose-dependently blocked dopamine uptake (54% reduction at 10 M) and amphetamine-stimulated efflux (59% reduction at 10M) in synaptosomes. It also produced a small but significant reduction in [H]WIN 35,428 binding in striatal membranes, indicating a weak interaction with the substrate binding site in the DAT. Biotinylation and cysteine accessibility studies indicated that tamoxifen stabilizes the outward-facing conformation of the DAT in a cocaine-like manner and does not affect surface expression of the DAT. Additional studies with mutant DAT constructs D476A and I159A suggested a direct interaction between tamoxifen and a secondary substrate binding site of the transporter. Locomotor studies revealed that tamoxifen attenuates amphetamine-stimulated hyperactivity in rats but has no depressant or stimulant activity in the absence of amphetamine. These results suggest a complex mechanism of action for tamoxifen as a regulator of the DAT. Due to its effectiveness against amphetamine actions and its central nervous system permeant activity, the tamoxifen structure represents an excellent starting point for a structure-based drug-design program to develop a pharmacological therapeutic for psychostimulant abuse.

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“…In a recent study, Mikelman et al show that tamoxifen interacts with the dopamine transporter (DAT) and can block amphetamine-stimulated dopamine release as well as blocking dopamine reuptake in rat synaptosomes (Mikelman et al 2018). While acute tamoxifen exposure did not change locomotor behavior, it was effective at blocking the locomotor-stimulating effects of amphetamine (Mikelman et al 2017;Mikelman et al 2018). It is possible that the neonatal DAT stimulation by tamoxifen caused the mild hyperactivity when the mice were tested as adults, though it is also possible that modulation of the estrogen receptor played a role.…”

Section: Discussionmentioning

confidence: 99%

Deletion of the creatine transporter gene in neonatal, but not adult, mice lead to cognitive deficits

Udobi

Delcimmuto

Kokenge

et al. 2019

Preprint

View full text Add to dashboard Cite

Creatine (Cr) is a guanidino compound that provides readily-available phosphate pools for the regeneration of spent ATP. The lack of brain Cr causes moderate to severe intellectual disability, language impairment, and epilepsy. The most prevalent cause of Cr deficiency are mutations in the X-linkedSLC6A8(Creatine transporter; CrT) gene, known as CrT deficiency (CTD). There are no current treatments for CTD and the mechanisms that underlie the cognitive deficits are poorly understood. One of the most critical areas that need to be addressed is if Cr is necessary for brain development. To address this concern, theSlc6a8gene was knocked out in either neonatal (postnatal day (P)5) or adult (P60) mice. The P5 knockout mice showed deficits in the Morris water maze and novel object recognition, while there were no deficits in P60 knockout mice. Interestingly, the P5 knockout mice showed hyperactivity during the dark phase; however, when examining control mice, the effect was due to the administration of tamoxifen from P5-10. Taken together, the results of this study show that Cr is necessary during periods of brain development involved in spatial and object learning. This study also highlights the continued importance of using proper control groups for behavioral testing.Take-home messageThe learning and memory deficits seen in Slc6a8-deficient mice are likely due to the developmental loss of Cr.

show abstract

Tamoxifen and its active metabolites inhibit dopamine transporter function independently of the estrogen receptors

Cited by 9 publications

References 16 publications

Deletion of the creatine transporter gene in neonatal, but not adult, mice leads to cognitive deficits

Deletion of the creatine transporter gene in neonatal, but not adult, mice leads to cognitive deficits

Tamoxifen Directly Interacts with the Dopamine Transporter

Deletion of the creatine transporter gene in neonatal, but not adult, mice lead to cognitive deficits

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