Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2

Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2

The serine/threonine kinase CK2 (formerly known as casein kinase II) plays a crucial role in various CNS disorders and is highly expressed in various types of cancer. Therefore, inhibiting this key kinase could be promising for the treatment of these diseases. The CK2 holoenzyme is formed by the rec...

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Main Authors: Lukas Kröger, Sebastian Borgert, Miriam Lauwers, Michaela Steinkrüger, Joachim Jose, Markus Pietsch, Bernhard Wünsch
Format: Article
Language:English
Published: MDPI AG 2024-12-01
Series:Molecules
Subjects:
CK2
protein kinase
heterotetrameric enzyme
protein–protein interaction
enzyme inhibition
Levy reaction
Online Access:https://www.mdpi.com/1420-3049/30/1/63
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author Lukas Kröger
Sebastian Borgert
Miriam Lauwers
Michaela Steinkrüger
Joachim Jose
Markus Pietsch
Bernhard Wünsch
author_facet Lukas Kröger
Sebastian Borgert
Miriam Lauwers
Michaela Steinkrüger
Joachim Jose
Markus Pietsch
Bernhard Wünsch
author_sort Lukas Kröger
collection DOAJ
description The serine/threonine kinase CK2 (formerly known as casein kinase II) plays a crucial role in various CNS disorders and is highly expressed in various types of cancer. Therefore, inhibiting this key kinase could be promising for the treatment of these diseases. The CK2 holoenzyme is formed by the recruitment of two catalytically active CK2α and/or CK2α′ subunits by a regulatory CK2β dimer. Starting with the lead furocarbazole W16 (<b>4</b>) inhibiting the CK2α/CK2β interaction, analogous pyrrolocarbazoles were prepared and tested for their protein–protein interaction inhibition (PPII). The key step of the synthesis was a multicomponent Levy reaction of 2-(indolyl)acetate <b>6</b>, benzaldehydes <b>7</b>, and <i>N</i>-substituted maleimides <b>8</b>. Targeted modifications were performed by the saponification of the tetracyclic ester <b>9a</b>, followed by the coupling of the resulting acid <b>10</b> with diverse amines. The replacement of the O-atom of the lead furocarbazole <b>4</b> by an N-atom in pyrrolocarbazoles retained or even increased the inhibition of the CK2α/CK2β interaction. The large benzyloxazolidinyl moiety of <b>4</b> could be replaced by smaller <i>N</i>-substituents without the loss of the PPII. The introduction of larger substituents at the 2-position and/or at <i>p</i>-position of the phenyl moiety at the 10-position to increase the surface for the inhibition of the PPI did not enhance the inhibition of the CK2α/CK2β association. The strong inhibition of the CK2α/CK2β association by the histidine derivative (+)-<b>20a</b> (<i>K</i><sub>i</sub> = 6.1 µM) translated into a high inhibition of the kinase activity of the CK2 holoenzyme (CK2α<sub>2</sub>β<sub>2</sub>, IC<sub>50</sub> = 2.5 µM). Thus, <b>20a</b> represents a novel lead compound inhibiting CK2 via the inhibition of the association of the CK2α and Ck2β subunits.
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series Molecules
spelling doaj-art-e0a3481a90a04aafbc3dc9615970e8a42025-01-10T13:18:46ZengMDPI AGMolecules1420-30492024-12-013016310.3390/molecules30010063Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2Lukas Kröger0Sebastian Borgert1Miriam Lauwers2Michaela Steinkrüger3Joachim Jose4Markus Pietsch5Bernhard Wünsch6Institut für Pharmazeutische und Medizinische Chemie, Universität Münster, Corrensstraße 48, D-48149 Münster, GermanyInstitut für Pharmazeutische und Medizinische Chemie, Universität Münster, Corrensstraße 48, D-48149 Münster, GermanyInstitutes I & II of Pharmacology, Center of Pharmacology, Faculty of Medicine and University Hospital Cologne, University of Cologne, Gleueler Straße 24, D-50931 Cologne, GermanyInstitutes I & II of Pharmacology, Center of Pharmacology, Faculty of Medicine and University Hospital Cologne, University of Cologne, Gleueler Straße 24, D-50931 Cologne, GermanyInstitut für Pharmazeutische und Medizinische Chemie, Universität Münster, Corrensstraße 48, D-48149 Münster, GermanyInstitutes I & II of Pharmacology, Center of Pharmacology, Faculty of Medicine and University Hospital Cologne, University of Cologne, Gleueler Straße 24, D-50931 Cologne, GermanyInstitut für Pharmazeutische und Medizinische Chemie, Universität Münster, Corrensstraße 48, D-48149 Münster, GermanyThe serine/threonine kinase CK2 (formerly known as casein kinase II) plays a crucial role in various CNS disorders and is highly expressed in various types of cancer. Therefore, inhibiting this key kinase could be promising for the treatment of these diseases. The CK2 holoenzyme is formed by the recruitment of two catalytically active CK2α and/or CK2α′ subunits by a regulatory CK2β dimer. Starting with the lead furocarbazole W16 (<b>4</b>) inhibiting the CK2α/CK2β interaction, analogous pyrrolocarbazoles were prepared and tested for their protein–protein interaction inhibition (PPII). The key step of the synthesis was a multicomponent Levy reaction of 2-(indolyl)acetate <b>6</b>, benzaldehydes <b>7</b>, and <i>N</i>-substituted maleimides <b>8</b>. Targeted modifications were performed by the saponification of the tetracyclic ester <b>9a</b>, followed by the coupling of the resulting acid <b>10</b> with diverse amines. The replacement of the O-atom of the lead furocarbazole <b>4</b> by an N-atom in pyrrolocarbazoles retained or even increased the inhibition of the CK2α/CK2β interaction. The large benzyloxazolidinyl moiety of <b>4</b> could be replaced by smaller <i>N</i>-substituents without the loss of the PPII. The introduction of larger substituents at the 2-position and/or at <i>p</i>-position of the phenyl moiety at the 10-position to increase the surface for the inhibition of the PPI did not enhance the inhibition of the CK2α/CK2β association. The strong inhibition of the CK2α/CK2β association by the histidine derivative (+)-<b>20a</b> (<i>K</i><sub>i</sub> = 6.1 µM) translated into a high inhibition of the kinase activity of the CK2 holoenzyme (CK2α<sub>2</sub>β<sub>2</sub>, IC<sub>50</sub> = 2.5 µM). Thus, <b>20a</b> represents a novel lead compound inhibiting CK2 via the inhibition of the association of the CK2α and Ck2β subunits.https://www.mdpi.com/1420-3049/30/1/63CK2protein kinaseheterotetrameric enzymeprotein–protein interactionenzyme inhibitionLevy reaction
spellingShingle Lukas Kröger
Sebastian Borgert
Miriam Lauwers
Michaela Steinkrüger
Joachim Jose
Markus Pietsch
Bernhard Wünsch
Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
Molecules
CK2
protein kinase
heterotetrameric enzyme
protein–protein interaction
enzyme inhibition
Levy reaction
title Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
title_full Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
title_fullStr Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
title_full_unstemmed Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
title_short Structure–Activity Relationship Studies of Tetracyclic Pyrrolocarbazoles Inhibiting Heterotetrameric Protein Kinase CK2
title_sort structure activity relationship studies of tetracyclic pyrrolocarbazoles inhibiting heterotetrameric protein kinase ck2
topic CK2
protein kinase
heterotetrameric enzyme
protein–protein interaction
enzyme inhibition
Levy reaction
url https://www.mdpi.com/1420-3049/30/1/63
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