CB1 and CB2 receptors are novel molecular targets for Tamoxifen and 4OH-Tamoxifen

CB1 and CB2 receptors are novel molecular targets for Tamoxifen and 4OH-Tamoxifen

•Tamoxifen produces cytotoxicity via estrogen-receptor (ER) independent mechanisms.•Tamoxifen binds to CB1 and CB2 cannabinoid receptors and acts as an inverse agonist.•CB1 and CB2 receptors are novel molecular targets for Tamoxifen.•ER-independent effects for Tamoxifen may be mediated via CB1 and/o...

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Veröffentlicht in:Biochemical and biophysical research communications 2013-11, Vol.441 (2), p.339-343
Hauptverfasser: Prather, Paul L., FrancisDevaraj, FeAna, Dates, Centdrika R., Greer, Aleksandra K., Bratton, Stacie M., Ford, Benjamin M., Franks, Lirit N., Radominska-Pandya, Anna
Format: Artikel
Sprache:eng
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60 APPLIED LIFE SCIENCES
adenylate cyclase
agonists
AMP
Animals
Antagonist
Antineoplastic Agents - chemistry
Antineoplastic Agents - pharmacology
apoptosis
breast neoplasms
Cannabinoid receptors
Cannabinoids
Cell Membrane - chemistry
CHO Cells
Cricetulus
cytotoxicity
Drug action
Drug discovery
Drug Inverse Agonism
DRUGS
estrogen receptors
ESTROGENS
G-protein coupled receptors
G-proteins
GTP-ASES
GUANOSINE
HAMSTERS
Humans
Inverse agonist
MAMMARY GLANDS
metabolites
Mice
neoplasm cells
NEOPLASMS
OVARIES
patients
PHENOL
Protein Binding
Receptor, Cannabinoid, CB1 - agonists
Receptor, Cannabinoid, CB1 - chemistry
Receptor, Cannabinoid, CB2 - agonists
Receptor, Cannabinoid, CB2 - chemistry
RECEPTORS
Selective Estrogen Receptor Modulators - chemistry
Selective Estrogen Receptor Modulators - pharmacology
TAMOXIFEN
Tamoxifen - analogs & derivatives
Tamoxifen - chemistry
Tamoxifen - pharmacology
TOXICITY
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Zusammenfassung:•Tamoxifen produces cytotoxicity via estrogen-receptor (ER) independent mechanisms.•Tamoxifen binds to CB1 and CB2 cannabinoid receptors and acts as an inverse agonist.•CB1 and CB2 receptors are novel molecular targets for Tamoxifen.•ER-independent effects for Tamoxifen may be mediated via CB1 and/or CB2 receptors. Tamoxifen (Tam) is classified as a selective estrogen receptor modulator (SERM) and is used for treatment of patients with ER-positive breast cancer. However, it has been shown that Tam and its cytochrome P450-generated metabolite 4-hydroxy-Tam (4OH-Tam) also exhibit cytotoxic effects in ER-negative breast cancer cells. These observations suggest that Tam and 4OH-Tam can produce cytotoxicity via estrogen receptor (ER)-independent mechanism(s) of action. The molecular targets responsible for the ER-independent effects of Tam and its derivatives are poorly understood. Interestingly, similar to Tam and 4OH-Tam, cannabinoids have also been shown to exhibit anti-proliferative and apoptotic effects in ER-negative breast cancer cells, and estrogen can regulate expression levels of cannabinoid receptors (CBRs). Therefore, this study investigated whether CBRs might serve as novel molecular targets for Tam and 4OH-Tam. We report that both compounds bind to CB1 and CB2Rs with moderate affinity (0.9–3μM). Furthermore, Tam and 4OH-Tam exhibit inverse activity at CB1 and CB2Rs in membrane preparations, reducing basal G-protein activity. Tam and 4OH-Tam also act as CB1/CB2R-inverse agonists to regulate the downstream intracellular effector adenylyl cyclase in intact cells, producing concentration-dependent increases in intracellular cAMP. These results suggest that CBRs are molecular targets for Tam and 4OH-Tam and may contribute to the ER-independent cytotoxic effects reported for these drugs. Importantly, these findings also indicate that Tam and 4OH-Tam might be used as structural scaffolds for development of novel, efficacious, non-toxic cancer drugs acting via CB1 and/or CB2Rs.
ISSN:0006-291X
1090-2104
DOI:10.1016/j.bbrc.2013.10.057