Tamoxifen Isomers and Metabolites Exhibit Distinct Affinity and Activity at Cannabinoid Receptors: Potential Scaffold for Drug Development

Ford, Benjamin M.; Franks, Lirit N.; Radominska‐Pandya, Anna; Prather, Paul L.

doi:10.1371/journal.pone.0167240

Cited by 11 publications

(8 citation statements)

References 72 publications

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“…Although this and previous studies clearly demonstrate that SERM-scaffolds may be useful for synthesis of selective CB 1 and/or CB 2 cannabinoid ligands (Kumar and Song, 2013; Prather et al, 2013; Ford et al, 2016), before novel compounds can be useful therapeutically, drugs in this class must first be designed that lack ER affinity to prevent off-target effects. Importantly, RID-B is only a first generation of many ridaifen (RID) compounds that are tamoxifen derivatives, developed to reduce ER affinity, yet maintain cytotoxic effects in cancer (Shiina et al, 2008; Guo et al, 2013b).…”

Section: Discussionmentioning

confidence: 78%

“…Based on the structural similarity of RID-B to tamoxifen (Fig. 1), and our past reports that tamoxifen exhibits moderate affinity for cannabinoid receptors (Prather et al, 2013; Ford et al, 2016), a competition receptor-binding screen was conducted. From this initial binding screen, it was observed that RID-B (1 μM) produced > 50% displacement of the CB 1 /CB 2 radioligand [ 3 H]-CP-55,940 (0.2 nM) from human CB 1 and CB 2 receptors stably expressed in CHO cells.…”

Section: Resultsmentioning

confidence: 99%

“…Our laboratory and others have recently reported that several selective estrogen receptor modulators (SERMs) exhibit moderate affinity for cannabinoid receptors and act as inverse agonists (Kumar and Song, 2013; Prather et al, 2013; Ford et al, 2016). SERMs are agonists and antagonists at estrogen receptors (ERs) and have traditionally been used therapeutically to treat ER-positive breast cancer, post-menopausal conditions, and osteoporosis (Maximov et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

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The tamoxifen derivative ridaifen-B is a high affinity selective CB 2 receptor inverse agonist exhibiting anti-inflammatory and anti-osteoclastogenic effects

Franks

Ford

Fujiwara

et al. 2018

Toxicology and Applied Pharmacology

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Selective estrogen receptor modulators (SERMs) target estrogen receptors (ERs) to treat breast cancer and osteoporosis. Several SERMs exhibit anti-cancer activity not related to ERs. To discover novel anti-cancer drugs acting via ER-independent mechanisms, derivatives of the SERM tamoxifen, known as the "ridaifen" compounds, have been developed that exhibit reduced or no ER affinity, while maintaining cytotoxicity. Tamoxifen and other SERMs bind to cannabinoid receptors with moderate affinity. Therefore, ER-independent effects of SERMs might be mediated via cannabinoid receptors. This study determined whether RID-B, a first generation ridaifen compound, exhibits affinity and/or activity at CB and/or CB cannabinoid receptors. RID-B binds with high affinity (K = 43.7 nM) and 17-fold selectivity to CB over CB receptors. RID-B acts as an inverse agonist at CB receptors, modulating G-protein and adenylyl cyclase activity with potency values predicted by CB affinity. Characteristic of an antagonist, RID-B co-incubation produces a parallel-rightward shift in the concentration-effect curve of CB agonist WIN-55,212-2 to inhibit adenylyl cyclase activity. CB inverse agonists are reported to exhibit anti-inflammatory and anti-ostoeclastogenic effects. In LPS-activated macrophages, RID-B exhibits anti-inflammatory effects by reducing levels of nitric oxide (NO), IL-6 and IL-1α, but not TNFα. Only reduction of NO concentration by RID-B is mediated by cannabinoid receptors. RID-B also exhibits pronounced anti-osteoclastogenic effects, reducing the number of osteoclasts differentiating from primary bone marrow macrophages in a cannabinoid receptor-dependent manner. In summary, the tamoxifen derivative RID-B, developed with reduced affinity for ERs, is a high affinity selective CB inverse agonist with anti-inflammatory and anti-osteoclastogenic properties.

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Section: Discussionmentioning

confidence: 78%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The tamoxifen derivative ridaifen-B is a high affinity selective CB 2 receptor inverse agonist exhibiting anti-inflammatory and anti-osteoclastogenic effects

Franks

Ford

Fujiwara

et al. 2018

Toxicology and Applied Pharmacology

Self Cite

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“…Tamoxifen is an anti-estrogen drug used in the treatment of breast cancer. Hepatotoxicity is a commonly reported side effect of tamoxifen (Ford et al, 2016; Henderson et al, 2016; Khuroo et al, 2014; Lin et al, 2014; Tabassum et al, 2006; Villegas et al, 2016). In our study, mitochondrial impairment and disruption of cell membrane integrity were the main mechanisms of tamoxifen-induced toxicity.…”

Section: Discussionmentioning

confidence: 99%

High-content imaging assays on a miniaturized 3D cell culture platform

Joshi

Datar

et al. 2018

Toxicology in Vitro

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The majority of high-content imaging (HCI) assays have been performed on two-dimensional (2D) cell monolayers for its convenience and throughput. However, 2D-cultured cell models often do not represent the in vivo characteristics accurately and therefore reduce the predictability of drug toxicity/efficacy in vivo. Recently, three-dimensional (3D) cell-based HCI assays have been demonstrated to improve predictability, but its use is limited due to difficulty in maneuverability and low throughput in cell imaging. To alleviate these issues, we have developed miniaturized 3D cell culture on a micropillar/microwell chip and demonstrated high-throughput HCI assays for mechanistic toxicity. Briefly, Hep3B human hepatoma cell line was encapsulated in a mixture of alginate and fibrin gel on the micropillar chip, cultured in 3D, and exposed to six model compounds in the microwell chip for rapidly assessing mechanistic hepatotoxicity. Several toxicity parameters, including DNA damage, mitochondrial impairment, intracellular glutathione level, and cell membrane integrity were measured on the chip, and the IC values of the compounds at different readouts were determined to investigate the mechanism of toxicity. Overall, the Z' factors were between 0.6 and 0.8 for the HCI assays, and the coefficient of variation (CV) were below 20%. These results indicate high robustness and reproducibility of the HCI assays established on the miniaturized 3D cell culture chip. In addition, it was possible to determine the predominant mechanism of toxicity using the 3D HCI assays. Therefore, our miniaturized 3D cell culture coupled with HCI assays has great potential for high-throughput screening (HTS) of compounds and mechanistic toxicity profiling.

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“…Accumulation of ROS inside cells decreases the glutathione level resulting in oxidative stress and causes mitochondrial impairment leading to apoptosis (Cabezas, El‐Bachá, González, & Barreto, ; Jin et al., ; N. Li et al., ; Moon, Lee, Park, Geum, & Kim, ). Tamoxifen is an anticancer drug with hepatotoxicity as its commonly reported side effect (Ford, Franks, Radominska‐Pandya, & Prather, ; Henderson, Wendy, & Kim, ; Khuroo et al., ; Lin et al., ; Tabassum, Rehman, Banerjee, Raisuddin, & Parvez, ; Villegas et al., ). Mitochondrial impairment is known to be the main mechanism of tamoxifen‐induced toxicity (Lee, Kang, Lee, & Kim, ; Tabassum et al., ; Tolosa et al., ; Tolosa, Carmona, Castell, Gómez‐Lechón, & Donato, ).…”

Section: Commentarymentioning

confidence: 99%

High‐Throughput Assessment of Mechanistic Toxicity of Chemicals in Miniaturized 3D Cell Culture

et al. 2018

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High-content imaging (HCI) assays on two-dimensional (2D) cell cultures often do not represent in vivo characteristics accurately, thus reducing the predictability of drug toxicity/efficacy in vivo. On the other hand, conventional 3D cell cultures are relatively low throughput and possess difficulty in cell imaging. To address these limitations, a miniaturized 3D cell culture has been developed on a micropillar/microwell chip platform with human cells encapsulated in biomimetic hydrogels. Model compounds are used to validate human cell microarrays for high-throughput assessment of mechanistic toxicity. Main mechanisms of toxicity of compounds can be investigated by analyzing multiple parameters such as DNA damage, mitochondrial impairment, intracellular glutathione level, and cell membrane integrity. IC 50 values of these parameters can be determined and compared for the compounds to investigate the main mechanism of toxicity. This paper describes miniaturized HCI assays on 3D-cultured cell microarrays for high-throughput assessment of mechanistic profiles of compound-induced toxicity. C 2018 by John Wiley & Sons, Inc.Keywords: 3D cell culture r assay miniaturization r high-content imaging r mechanistic toxicity r microarray chip platform -Y (2019).High-throughput assessment of mechanistic toxicity of chemicals in miniaturized 3D cell culture.This protocol provides detailed steps involved in high-throughput cell printing with a bioprinter (S+ Microarrayer) for the generation of miniaturized 3D cell culture on a micropillar/microwell chip platform and the measurement of dose responses of model compounds in the miniaturized 3D culture of human cells using an automated fluorescent microscope (S+ Scanner) for HCI assays. Incorporating 3D cell growth on the chip platform in combination with HCI assays can be established as a reliable technique for testing toxicity of compounds in an early stage of preclinical drug discovery and better predict in vivo toxicity in clinical trials. The procedures provided below enable users to efficiently determine the mechanism of toxicity of unknown compounds in high-throughput and without the excessive use of cells, hydrogels, and other reagents. MaterialsHep3B human hepatoma cell line (ATCC# HB-8064, RRID:CVCL_0326) as a model cell line Complete RPMI-1640 medium for culturing Hep3B cells (see recipe) 1× phosphate-buffered saline (PBS; see recipe)Joshi et al.

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Tamoxifen Isomers and Metabolites Exhibit Distinct Affinity and Activity at Cannabinoid Receptors: Potential Scaffold for Drug Development

Cited by 11 publications

References 72 publications

The tamoxifen derivative ridaifen-B is a high affinity selective CB 2 receptor inverse agonist exhibiting anti-inflammatory and anti-osteoclastogenic effects

The tamoxifen derivative ridaifen-B is a high affinity selective CB 2 receptor inverse agonist exhibiting anti-inflammatory and anti-osteoclastogenic effects

High-content imaging assays on a miniaturized 3D cell culture platform

High‐Throughput Assessment of Mechanistic Toxicity of Chemicals in Miniaturized 3D Cell Culture

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