ABSTRACT
Bexarotene is an FDA-approved drug for the treatment of cutaneous T-cell lymphoma (CTCL); however, its use provokes or disrupts other retinoid-X-receptor (RXR)-dependent nuclear receptor pathways and thereby incites side effects including hypothyroidism and raised triglycerides. Two novel bexarotene analogs, as well as three unique CD3254 analogs and thirteen novel NEt-TMN analogs, were synthesized and characterized for their ability to induce RXR agonism in comparison to bexarotene (1). Several analogs in all three groups possessed an isochroman ring substitution for the bexarotene aliphatic group. Analogs were modeled for RXR binding affinity, and EC50 as well as IC50 values were established for all analogs in a KMT2A-MLLT3 leukemia cell line. All analogs were assessed for liver-X-receptor (LXR) activity in an LXRE system to gauge the potential for the compounds to provoke raised triglycerides by increasing LXR activity, as well as to drive LXRE-mediated transcription of brain ApoE expression as a marker for potential therapeutic use in neurodegenerative disorders. Preliminary results suggest these compounds display a broad spectrum of off-target activities. However, many of the novel compounds were observed to be more potent than 1. While some RXR agonists cross-signal the retinoic acid receptor (RAR), many of the rexinoids in this work displayed reduced RAR activity. The isochroman group did not appear to substantially reduce RXR activity on its own. The results of this study reveal that modifying potent, selective rexinoids like bexarotene, CD3254, and NEt-TMN can provide rexinoids with increased RXR selectivity, decreased potential for cross-signaling, and improved anti-proliferative characteristics in leukemia models compared to 1.
Subject(s)
Leukemia , Lymphoma, T-Cell, Cutaneous , Skin Neoplasms , Humans , Bexarotene/pharmacology , Retinoid X Receptors/metabolism , Tetrahydronaphthalenes/pharmacology , Liver X Receptors , Retinoids/pharmacology , TriglyceridesABSTRACT
The synthesis of trimethylsilyl (TMS) hydroperoxide derivatives for gas chromatography (GC) was studied using N-methyl-N-(trimethylsilyl) trifluoroacetamide (MSTFA) for derivatization of cumene hydroperoxide (CMOOH) (alpha,alpha'-dimethylbenzyl hydroperoxide) and alpha-methoxyalkyl hydroperoxides formed by liquid- and gas-phase ozonolysis of a series of terminal alkenes in the presence of methanol (CH3OH). Derivatization efficiencies >90% were achieved over a wide range of solution concentrations. The major compounds identified by GC-mass spectrometry of the derivatized products of alkene-O3 reactions were alpha-methoxyalkyl hydroperoxides, methyl esters, and aldehydes. Yields of alpha-methoxyalkyl hydroperoxides and methyl esters were quantified using effective carbon numbers (ECNs) and used to determine the yields of stabilized Criegee intermediates (SCIs) from gas-phase ozonolysis reactions. Such measurements are important for understanding the atmospheric chemistry of alkene emissions. SCI yields measured for the reactions of 1-octene [CH3(CH2)5CH=CH2], 1-nonene [CH3(CH2)6CH=CH2 ], and 2-methyl-1-octene [CH3(CH2)5C(CH3)=CH2] are consistent with previous measurements or predictions based on literature data. SCI yields measured for the reactions of 1-decene [CH3(CH2)7CH=CH2], 1-dodecene [CH3 (CH2)9CH=CH2], and 1-tetradecene [CH3(CH2)11CH=CH2] are much lower than expected, apparently due to side reactions with low volatility aldehydes that form peroxyhemiacetals, which are not amenable to GC analysis. In general, the results indicate that off-line MSTFA derivatization can be an efficient means for increasing the stability of thermally labile hydroperoxides for identification and quantitation by GC, and offers a new approach for the analysis of these environmentally important compounds.
