Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family

We performed an X-ray crystallographic study of complexes of protein kinase PIM-1 with three inhibitors comprising an adenosine mimetic moiety, a linker, and a peptide-mimetic (d-Arg)(6) fragment. Guided by the structural models, simplified chemical structures with a reduced number of polar groups a...

Descripción completa

Detalles Bibliográficos
Autores principales: Nonga, Olivier E., Lavogina, Darja, Enkvist, Erki, Kestav, Katrin, Chaikuad, Apirat, Dixon-Clarke, Sarah E., Bullock, Alex N., Kopanchuk, Sergei, Ivan, Taavi, Ekambaram, Ramesh, Viht, Kaido, Knapp, Stefan, Uri, Asko
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8307404/
https://www.ncbi.nlm.nih.gov/pubmed/34299628
http://dx.doi.org/10.3390/molecules26144353
_version_ 1783728038414909440
author Nonga, Olivier E.
Lavogina, Darja
Enkvist, Erki
Kestav, Katrin
Chaikuad, Apirat
Dixon-Clarke, Sarah E.
Bullock, Alex N.
Kopanchuk, Sergei
Ivan, Taavi
Ekambaram, Ramesh
Viht, Kaido
Knapp, Stefan
Uri, Asko
author_facet Nonga, Olivier E.
Lavogina, Darja
Enkvist, Erki
Kestav, Katrin
Chaikuad, Apirat
Dixon-Clarke, Sarah E.
Bullock, Alex N.
Kopanchuk, Sergei
Ivan, Taavi
Ekambaram, Ramesh
Viht, Kaido
Knapp, Stefan
Uri, Asko
author_sort Nonga, Olivier E.
collection PubMed
description We performed an X-ray crystallographic study of complexes of protein kinase PIM-1 with three inhibitors comprising an adenosine mimetic moiety, a linker, and a peptide-mimetic (d-Arg)(6) fragment. Guided by the structural models, simplified chemical structures with a reduced number of polar groups and chiral centers were designed. The developed inhibitors retained low-nanomolar potency and possessed remarkable selectivity toward the PIM kinases. The new inhibitors were derivatized with biotin or fluorescent dye Cy5 and then applied for the detection of PIM kinases in biochemical solutions and in complex biological samples. The sandwich assay utilizing a PIM-2-selective detection antibody featured a low limit of quantification (44 pg of active recombinant PIM-2). Fluorescent probes were efficiently taken up by U2OS cells and showed a high extent of co-localization with PIM-1 fused with a fluorescent protein. Overall, the developed inhibitors and derivatives represent versatile chemical tools for studying PIM function in cellular systems in normal and disease physiology.
format Online
Article
Text
id pubmed-8307404
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-83074042021-07-25 Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family Nonga, Olivier E. Lavogina, Darja Enkvist, Erki Kestav, Katrin Chaikuad, Apirat Dixon-Clarke, Sarah E. Bullock, Alex N. Kopanchuk, Sergei Ivan, Taavi Ekambaram, Ramesh Viht, Kaido Knapp, Stefan Uri, Asko Molecules Article We performed an X-ray crystallographic study of complexes of protein kinase PIM-1 with three inhibitors comprising an adenosine mimetic moiety, a linker, and a peptide-mimetic (d-Arg)(6) fragment. Guided by the structural models, simplified chemical structures with a reduced number of polar groups and chiral centers were designed. The developed inhibitors retained low-nanomolar potency and possessed remarkable selectivity toward the PIM kinases. The new inhibitors were derivatized with biotin or fluorescent dye Cy5 and then applied for the detection of PIM kinases in biochemical solutions and in complex biological samples. The sandwich assay utilizing a PIM-2-selective detection antibody featured a low limit of quantification (44 pg of active recombinant PIM-2). Fluorescent probes were efficiently taken up by U2OS cells and showed a high extent of co-localization with PIM-1 fused with a fluorescent protein. Overall, the developed inhibitors and derivatives represent versatile chemical tools for studying PIM function in cellular systems in normal and disease physiology. MDPI 2021-07-19 /pmc/articles/PMC8307404/ /pubmed/34299628 http://dx.doi.org/10.3390/molecules26144353 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Nonga, Olivier E.
Lavogina, Darja
Enkvist, Erki
Kestav, Katrin
Chaikuad, Apirat
Dixon-Clarke, Sarah E.
Bullock, Alex N.
Kopanchuk, Sergei
Ivan, Taavi
Ekambaram, Ramesh
Viht, Kaido
Knapp, Stefan
Uri, Asko
Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title_full Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title_fullStr Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title_full_unstemmed Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title_short Crystal Structure-Guided Design of Bisubstrate Inhibitors and Photoluminescent Probes for Protein Kinases of the PIM Family
title_sort crystal structure-guided design of bisubstrate inhibitors and photoluminescent probes for protein kinases of the pim family
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8307404/
https://www.ncbi.nlm.nih.gov/pubmed/34299628
http://dx.doi.org/10.3390/molecules26144353
work_keys_str_mv AT nongaoliviere crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT lavoginadarja crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT enkvisterki crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT kestavkatrin crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT chaikuadapirat crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT dixonclarkesarahe crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT bullockalexn crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT kopanchuksergei crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT ivantaavi crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT ekambaramramesh crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT vihtkaido crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT knappstefan crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily
AT uriasko crystalstructureguideddesignofbisubstrateinhibitorsandphotoluminescentprobesforproteinkinasesofthepimfamily

Ejemplares similares