BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Metabolism of nitric oxide, Vitamin E, rs2300478, MYC, cell-cell adhesion, Influenza)
Bookmark Forward

Novel σ1 antagonists designed for tumor therapy: Structure - activity relationships of aminoethyl substituted cyclohexanes.

Nicole Kopp, Catharina Holtschulte, Frederik Börgel, Kirstin Lehmkuhl, Kristina Friedland, Gianluca Civenni, Erik Laurini, Carlo V Catapano, Sabrina Pricl, Hans-Ulrich Humpf, Dirk Schepmann, Bernhard Wünsch

European journal of medicinal chemistry 2021 Jan 15


filter terms:
  • 1 receptor (1)
  • adduct (1)
  • cyclohexanes (3)
  • human cell (2)
  • humans (1)
  • inhibit (2)
  • liver (1)
  • mice (1)
  • nadph (1)
  • parent (1)
  • prostate (1)
  • receptor (2)
  • receptor (3)
    • Sizes of these terms reflect their relevance to your search.

    Depending on the substitution pattern and stereochemistry, 1,3-dioxanes 1 with an aminoethyl moiety in 4-position represent potent σ1 receptor antagonists. In order to increase the stability, a cyclohexane ring first replaced the acetalic 1, 3-dioxane ring of 1. A large set of aminoethyl substituted cyclohexane derivatives was prepared in a six-step synthesis. All enantiomers and diastereomers were separated by chiral HPLC at the stage of the primary alcohol 7, and their absolute configuration was determined by CD spectroscopy. Neither the relative nor the absolute configuration had a large impact on the σ1 affinity. The highest σ1 affinity was found for cis-configured benzylamines (1R,3S)-11 (Ki = 0.61 nM) and (1S,3R)-11 (Ki = 1.3 nM). Molecular dynamics simulations showed that binding of (1R,3S)-11 at the σ1 receptor is stabilized by the typical polar interaction of the protonated amino moiety with the carboxy group of E172 which is optimally oriented by an H-bond interaction with Y103. The lipophilic interaction of I124 with the N-substituent also contributes to the high σ1 affinity of the benzylamines. The antagonistic activity was determined in a Ca2+ influx assay in retinal ganglion cells. The enantiomeric cis-configured benzylamines (1R,3S)-11 and (1S,3R)-11 were able to inhibit the growth of DU145 cells, a highly aggressive human prostate tumor cell line. Moreover, cis-11 could also inhibit the growth of further human tumor cells expressing σ1 receptors. The experimentally determined logD7.4 value of 3.13 for (1R,3S)-11 is in a promising range regarding membrane penetration. After incubation with mouse liver microsomes and NADPH for 90 min, 43% of the parent (1R,3S)-11 remained unchanged, indicating intermediate metabolic stability. Altogether, nine metabolites including one glutathione adduct were detected by means of LC-MS analysis. Copyright © 2020 Elsevier Masson SAS. All rights reserved.

    Citation

    Nicole Kopp, Catharina Holtschulte, Frederik Börgel, Kirstin Lehmkuhl, Kristina Friedland, Gianluca Civenni, Erik Laurini, Carlo V Catapano, Sabrina Pricl, Hans-Ulrich Humpf, Dirk Schepmann, Bernhard Wünsch. Novel σ1 antagonists designed for tumor therapy: Structure - activity relationships of aminoethyl substituted cyclohexanes. European journal of medicinal chemistry. 2021 Jan 15;210:112950

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 33148494

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.