Modeling, Synthesis, and Biological Evaluation of Potential Retinoid X Receptor (RXR) Selective Agonists: Novel Analogues of 4-[1-(3,5,5,8,8-Pentamethyl-5,6,7,8-tetrahydro-2-naphthyl)ethynyl]benzoic Acid (Bexarotene) and (<i>E</i>)-3-(3-(1,2,3,4-tetrahydro-1,1,4,4,6-pentamethylnaphthalen-7-yl)-4-hydroxyphenyl)acrylic Acid (CD3254)

Jurutka, Peter W.; Kaneko, Ichiro; Yang, Joanna C.; Bhogal, Jaskaran S.; Swierski, Johnathon C.; Tabacaru, Christa; Montano, Luis A.; Huynh, Chanh C.; Jama, Rabia A.; Mahelona, Ryan D.; Sarnowski, Joseph T.; Marcus, Lisa M.; Quezada, Alexis; Lemming, Brittney; Tedesco, Maria A.; Fischer, Audra J.; Mohamed, Saïd; Ma, Ning; Gray, Geoffrey; Vaart, Arjan van der; Marshall, Pamela A.; Wagner, Carl E.

doi:10.1021/jm4008517

Cited by 24 publications

(32 citation statements)

References 75 publications

(200 reference statements)

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“…; Jurutka et al. ), and EC 50 s comparable to bexarotene (Table ) can be synthesized that, with the correct chemistry and binding profile, may alleviate or minimize thyroid hormone axis side effects. At a concentration of 1 × 10 −7 mol/L, compounds 2 , 5 , 6 , 7 , 10 , 11 , 12 , 13 , and 14 demonstrate at least 85% (or more) of the activity of T3 alone (second bar from left), with less inhibition than 1 (bexarotene), and indeed 2 , 5 , 6 , 7 , 10 , 12 , and 13 are statistically the same as T3 alone (using a two‐tailed heteroscedastic t ‐test).…”

Section: Resultsmentioning

confidence: 99%

“…; Jurutka et al. ). The cells were cotransfected using a human RXR binding domain (BD) vector, a human RXR activation domain (AD) vector, a luciferase reporter gene containing BD‐binding sites, and Renilla control plasmid, using 2 μ L/well of Express‐IN transfection reagent (Thermo Fisher Scientific, Lafayette, CO) that was allowed to incubate for 24 h with the cells.…”

Section: Methodsmentioning

confidence: 97%

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Analysis of differential secondary effects of novel rexinoids: select rexinoid X receptor ligands demonstrate differentiated side effect profiles

Marshall

Jurutka

Wagner

et al. 2015

Pharmacology Res & Perspec

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In order to determine the feasibility of utilizing novel rexinoids for chemotherapeutics and as potential treatments for neurological conditions, we undertook an assessment of the side effect profile of select rexinoid X receptor (RXR) analogs that we reported previously. We assessed pharmacokinetic profiles, lipid and thyroid-stimulating hormone (TSH) levels in rats, and cell culture activity of rexinoids in sterol regulatory element-binding protein (SREBP) induction and thyroid hormone inhibition assays. We also performed RNA sequencing of the brain tissues of rats that had been dosed with the compounds. We show here for the first time that potent rexinoid activity can be uncoupled from drastic lipid changes and thyroid axis variations, and we propose that rexinoids can be developed with improved side effect profiles than the parent compound, bexarotene (1).

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 97%

Analysis of differential secondary effects of novel rexinoids: select rexinoid X receptor ligands demonstrate differentiated side effect profiles

Marshall

Jurutka

Wagner

et al. 2015

Pharmacology Res & Perspec

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“…This molecule presented an EC 50 value of 34 nM in HCT‐116 colon cancer cells, which is superior to the EC 50 value for 2 , 55 nM . The acrylic acid analogue CD3254 ( 20 ) was also reported as a potent and selective RXR agonist (EC 50 = 13 ± 3 nM in HCT‐116 cells) . Another set of similar molecules reported by the group of Jurutka, compounds 21 to 24 , appear to be more potent, demonstrate higher efficacy, and are likely to cause side effects than 2 .…”

Section: Rxr Agonistsmentioning

confidence: 85%

“…An apoptotic assay of treated CTCL cells using sodium butyrate as a control (100% dead) indicated that, after treatment with 100 nM of the compounds, 2 and molecules 22 to 24 killed ~50% of the cells while 21 caused ~70% cell death. The results also indicated that modification of 2 with more polar atoms in the aromatic ring that bears the carboxylic acid may increase the ability to activate RAR (% RAR agonistic activity at 100 nM = 27 ± 6, 28 ± 5, 31 ± 6, and 24 ± 4 for 21 to 24 in transfected HCT‐116 cells, respectively) and the ability to activate RXR (analogue 21 ) …”

Section: Rxr Agonistsmentioning

confidence: 95%

“…The acrylic acid analogue CD3254 ( 20 ) was also reported as a potent and selective RXR agonist (EC 50 = 13 ± 3 nM in HCT‐116 cells) . Another set of similar molecules reported by the group of Jurutka, compounds 21 to 24 , appear to be more potent, demonstrate higher efficacy, and are likely to cause side effects than 2 . The analogues 21 (EC 50 = 44 ± 12 nM), 22 (EC 50 = 50 ± 10 nM), 23 (EC 50 = 42 ± 3 nM), and 24 (EC 50 = 15 ± 2 nM) showed RXR activity compared with 2, EC 50 = 55 ± 6, in transfected HCT‐116 cells, demonstrating that improvements in potency and selectivity of 2 can be achieved through drug design.…”

Section: Rxr Agonistsmentioning

confidence: 97%

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A review of the molecular design and biological activities of RXR agonists

Almeida

Conda‐Sheridan

2019

Medicinal Research Reviews

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An attractive approach to combat disease is to target theregulation of cell function. At the heart of this task are nuclear receptors (NRs); which control functions such as gene transcription. Arguably, the key player in this regulatory machinery is the retinoid X receptor (RXR). This NR associates with a third of the NRs found in humans. Scientists have hypothesized that controlling the activity of RXR is an attractive approach to control cellular functions that modulate diseases such as cancer, diabetes, Alzheimer's disease and Parkinson's disease. In this review, we will describe the key features of the RXR, present a historic perspective of the first RXR agonists, and discuss various templates that have been reported to activate RXR with a focus on their molecular structure, biological activity, and limitations. Finally, we will present an outlook of the field and future directions and considerations to synthesize or modulate RXR agonists to make these compounds a clinical reality.

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Identifying the receptor subtype selectivity of retinoid X and retinoic acid receptors via quantum mechanics

Tsuji¹,

Shudo

Kagechika

2017

FEBS Open Bio

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Understanding and identifying the receptor subtype selectivity of a ligand is an important issue in the field of drug discovery. Using a combination of classical molecular mechanics and quantum mechanical calculations, this report assesses the receptor subtype selectivity for the human retinoid X receptor (hRXR) and retinoic acid receptor (hRAR) ligand‐binding domains (LBDs) complexed with retinoid ligands. The calculated energies show good correlation with the experimentally reported binding affinities. The technique proposed here is a promising method as it reveals the origin of the receptor subtype selectivity of selective ligands.

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Cited by 24 publications

References 75 publications

Analysis of differential secondary effects of novel rexinoids: select rexinoid X receptor ligands demonstrate differentiated side effect profiles

Analysis of differential secondary effects of novel rexinoids: select rexinoid X receptor ligands demonstrate differentiated side effect profiles

A review of the molecular design and biological activities of RXR agonists

Identifying the receptor subtype selectivity of retinoid X and retinoic acid receptors via quantum mechanics

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