Isoform-Selective HDAC Inhibition in Autoimmune DiseaseNicole L Regna1* and Christopher M Reilly2

Regna, Nicole L.; Reilly, Christopher M.

doi:10.4172/2155-9899.1000207

Cited by 5 publications

(10 citation statements)

References 122 publications

(131 reference statements)

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“…[10][11][12][13] Partly,this interest is driven by practical issues,asmechanical considerations affect the stability of molecular solids across ad iverse range of applications,from pharmaceuticals [3,[14][15][16] to energetic materials. [4,5] But the research is also driven by basic science,assome molecular solids exhibit Youngs moduli much higher than that expected from naive considerations.…”

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confidence: 99%

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Unusually Large Young’s Moduli of Amino Acid Molecular Crystals

et al. 2015

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Young's moduli of selected amino acid molecular crystals were studied both experimentally and computationally using nanoindentation and dispersion-corrected density functional theory. The Young modulus is found to be strongly facet-dependent, with some facets exhibiting exceptionally high values (as large as 44 GPa). The magnitude of Young's modulus is strongly correlated with the relative orientation between the underlying hydrogen-bonding network and the measured facet. Furthermore, we show computationally that the Young modulus can be as large as 70-90 GPa if facets perpendicular to the primary direction of the hydrogen-bonding network can be stabilized. This value is remarkably high for a molecular solid and suggests the design of hydrogen-bond networks as a route for rational design of ultra-stiff molecular solids.

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confidence: 99%

“…[43] Thec omputed Youngs moduli obtained along the experimentally accessible crystallographic directions,aswell as the minimum and maximum values,are given in Table 1. Three-dimensional renderings of the anisotropy of Youngs moduli [41,14] are given in Figure 2.…”

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Unusually Large Young’s Moduli of Amino Acid Molecular Crystals

et al. 2015

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“…HATs attach acetyl groups to lysine residues in histone and nonhistone proteins which provoke transcriptional activities, while HDACs catalyze the removal of acetyl groups causing chromatin to become highly packaged and, therefore, resulting in repressed gene expression . Overexpression of these enzymes correlate with several diseases including cancer, inflammation, neurodegenerative, and metabolic disorders . Therefore, histone deacetylase inhibitors represent an effective way to prevent the dysregulation of HDACs …”

Section: Introductionmentioning

confidence: 99%

Enantioselective synthesis and biological investigation of tetrahydro‐β‐carboline‐based HDAC6 inhibitors with improved solubility

Grünstein

Sellmer

Mahboobi

2019

Archiv der Pharmazie

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Aberrant epigenetic changes in DNA methylation and histone modification by acetylation or deacetylation regulate the pathogenesis of many diseases. Especially selective inhibitors are getting more and more attention. We recently reported on a new class of potent and selective anti-inflammatory and antirheumatic histone deacetylase 6 (HDAC6) inhibitors (e.g., Marbostat-100). The attachment of a morpholinoethoxy part to the head group dramatically enhances the solubility, in particular the solubility in aqueous solutions, of the lead compound Marbostat-100.Here, we present the enantioselective synthesis of small-molecule compounds based on the tetrahydro-β-carboline core system with improved solubility, and the influence of the stereochemistry on the biological activity. The enantiomers were synthesized in good enantiomeric excess (ee) purity and were potent and selective HDAC6 inhibitors, whereas the S-derivative S-21 is clearly the eutomer. The potency of our selective HDAC6 inhibitors is demonstrated by K i values in the range of 0.5-2 nM toward HDAC6, and the selectivity was proved in cellular assays by Western blot analysis taking ac-tubulin as surrogate parameter.

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“…Histone deacetylation assists the condensation of chromatin which further promotes transcriptional repression. HDAC inhibitors (HDACIs) have been identified as anticancer agents (Drummond et al, 2005;Guha, 2015;Mottamal, Zheng, Huang, & Wang, 2015;Qiao et al, 2013), immune modulators (Adcock, Ito, & Barnes, 2005;Choi & Reddy, 2011;Dinarello, Fossati, & Mascagni, 2011;Faraco, Cavone, & Chiarugi, 2011;Halili, Andrews, Sweet, & Fairlie, 2009;Huber et al, 2007;Kawabata et al, 2010;Leoni et al, 2005;Perl, 2010;Reddy et al, 2008;Regna & Reilly, 2014;Reilly, Regna, & Mishra, 2011;Villeneuve & Natarajan, 2010;Woan, Sahakian, Sotomayor, Seto, & Villagra, 2012) and are useful in neurodegenerative disorders (Abel & Zukin, 2008;Kazantsev & Thompson, 2008). Till date, 18 individual HDACs have been identified, which are classified into four major classes based on their sequence similarity to yeast counterpart (Dokmanovic, Clarke, & Marks, 2007).…”

Section: Introductionmentioning

confidence: 99%

Combined comparative molecular field analysis, comparative molecular similarity indices analysis, molecular docking and molecular dynamics studies of histone deacetylase 6 inhibitors

et al. 2019

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Human histone deacetylase isoform 6 (HDAC6) has been shown to have an immense role in cell motility and aggresome formation and is being an attractive selective target for the treatment of multiple tumour types and neurodegenerative conditions. The discovery of selective HDAC6 inhibitors with new chemical functionalities is therefore of utmost interest to researchers. In order to examine the structural requirements for HDAC6‐specific inhibitors and to derive predictive model which can be used for designing new selective HDAC6 inhibitors, a three‐dimensional quantitative structure–activity relationship study was carried out on a diverse set of ligands using common feature‐based pharmacophore alignment followed by employing comparative molecular field analysis (CoMFA) and comparative molecular similarity indices analysis (CoMSIA) techniques. The models displayed high correlation of 0.978 and 0.991 for best CoMFA and CoMSIA models, respectively, and a good statistical significance. The model could be used for predicting activities of the test set compounds as well as for deriving useful information regarding steric, electrostatic, hydrophobic properties of the molecules used in this study. Further, the training and test set molecules were docked into the HDAC6 binding site and molecular dynamics was carried out to suggest structural requirements for design of new inhibitors.

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Isoform-Selective HDAC Inhibition in Autoimmune DiseaseNicole L Regna1* and Christopher M Reilly2

Cited by 5 publications

References 122 publications

Unusually Large Young’s Moduli of Amino Acid Molecular Crystals

Unusually Large Young’s Moduli of Amino Acid Molecular Crystals

Enantioselective synthesis and biological investigation of tetrahydro‐β‐carboline‐based HDAC6 inhibitors with improved solubility

Combined comparative molecular field analysis, comparative molecular similarity indices analysis, molecular docking and molecular dynamics studies of histone deacetylase 6 inhibitors

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