2015
DOI: 10.1016/j.bmc.2015.01.049
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Structure–activity study for (bis)ureidopropyl- and (bis)thioureidopropyldiamine LSD1 inhibitors with 3-5-3 and 3-6-3 carbon backbone architectures

Abstract: Methylation at specific histone lysine residues is a critical post-translational modification that alters chromatin architecture, and dysregulated lysine methylation/demethylation is associated with the silencing of tumor suppressor genes. The enzyme lysine-specific demethylase 1 (LSD1) complexed to specific transcription factors catalyzes the oxidative demethylation of mono- and dimethyllysine 4 of histone H3 (H3K4me and H3K4me2 respectively). We have previously reported potent (bis)urea and (bis)thiourea LSD… Show more

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Cited by 42 publications
(25 citation statements)
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“…Therefore, the polyamine analogs provided the first proof of principle that LSD1 could be targeted as an anticancer strategy both in vitro and in vivo [102,103]. Efforts continue to improve upon this paradigm with the goal of designing more selective and potent inhibitors of LSD1 that have the added benefit of being targeting to chromatin [104107]. Although the polyamine analogs targeting LSD1 were first into this new pharmacologic space for cancer therapy, none have yet made it into the clinical trial.…”
Section: Targeting Polyamine Metabolism As An Anticancer Strategymentioning
confidence: 99%
“…Therefore, the polyamine analogs provided the first proof of principle that LSD1 could be targeted as an anticancer strategy both in vitro and in vivo [102,103]. Efforts continue to improve upon this paradigm with the goal of designing more selective and potent inhibitors of LSD1 that have the added benefit of being targeting to chromatin [104107]. Although the polyamine analogs targeting LSD1 were first into this new pharmacologic space for cancer therapy, none have yet made it into the clinical trial.…”
Section: Targeting Polyamine Metabolism As An Anticancer Strategymentioning
confidence: 99%
“…The (bis)ureido- and (bis)thioureido diamines 1 – 12 described in this article were synthesized according to our recently published pathway, 18 as shown in Scheme 1. The synthesis of compound 3 is described below, and all other compounds were synthesized in exactly the same manner.…”
Section: Chemistrymentioning
confidence: 99%
“…Other compounds beyond tranylcypromine and phenelzine analogs have been reported as LSD1 inhibitors including polyamines (Nowotarski et al, 2015) and hydrazone HCI-2509 but whose specificity and mechanisms of inhibition remain less well characterized (Wang, Huang, et al, 2015). Given that many of the in vitro LSD1 demethylase assays employ peroxidase as an indirect measure of LSD1 enzymatic activity, and the peroxidase activity can be interfered with by particular compounds, it is critical to use secondary assays such as mass spectrometry analysis that directly monitors peptide methylation status to ensure the reliability of a particular LSD1 inhibitor finding.…”
Section: Inhibitors Of Lsd1mentioning
confidence: 99%