Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK

MK5 (MAPK-activated protein kinase 5) or PRAK (p38-regulated and -activated kinase) are alternative names for a serine/threonine protein kinase downstream to ERK3/4 and p38 MAPK. A previous gene targeting approach for MK5/PRAK (termed here MK5/PRAK-Δex8) revealed a seemingly tumor-suppressive role o...

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Autores principales: Ronkina, Natalia, Johansen, Claus, Bohlmann, Lisa, Lafera, Juri, Menon, Manoj B., Tiedje, Christopher, Laaß, Kathrin, Turk, Benjamin E., Iversen, Lars, Kotlyarov, Alexey, Gaestel, Matthias
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4546416/
https://www.ncbi.nlm.nih.gov/pubmed/26295581
http://dx.doi.org/10.1371/journal.pone.0136138
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author Ronkina, Natalia
Johansen, Claus
Bohlmann, Lisa
Lafera, Juri
Menon, Manoj B.
Tiedje, Christopher
Laaß, Kathrin
Turk, Benjamin E.
Iversen, Lars
Kotlyarov, Alexey
Gaestel, Matthias
author_facet Ronkina, Natalia
Johansen, Claus
Bohlmann, Lisa
Lafera, Juri
Menon, Manoj B.
Tiedje, Christopher
Laaß, Kathrin
Turk, Benjamin E.
Iversen, Lars
Kotlyarov, Alexey
Gaestel, Matthias
author_sort Ronkina, Natalia
collection PubMed
description MK5 (MAPK-activated protein kinase 5) or PRAK (p38-regulated and -activated kinase) are alternative names for a serine/threonine protein kinase downstream to ERK3/4 and p38 MAPK. A previous gene targeting approach for MK5/PRAK (termed here MK5/PRAK-Δex8) revealed a seemingly tumor-suppressive role of MK5/PRAK in DMBA-induced one step skin carcinogenesis and Ras-induced transformation. Here we demonstrate that an alternative targeting strategy of MK5/PRAK (termed MK5/PRAK-Δex6) increased neither tumor incidence in the one step skin carcinogenesis model, nor Ras-induced transformation in primary cells. Interestingly, due to the targeting strategies and exon skipping both knockouts do not completely abolish the generation of MK5/PRAK protein, but express MK5/PRAK deletion mutants with different biochemical properties depending on the exon targeted: Targeting of exon 6 leads to expression of an unstable cytoplasmic catalytically inactive MK5/PRAK-Δex6 mutant while targeting of exon 8 results in a more stable nuclear MK5/PRAK-Δex8 mutant with residual catalytic activity. The different properties of the MK5/PRAK deletion mutants could be responsible for the observed discrepancy between the knockout strains and challenge the role of MK5/PRAK in p53-dependent tumor suppression. Further MK5/PRAK knockout and knock-in mouse strains will be necessary to assign a physiological function to MK5/PRAK in this model organism.
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spelling pubmed-45464162015-09-01 Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK Ronkina, Natalia Johansen, Claus Bohlmann, Lisa Lafera, Juri Menon, Manoj B. Tiedje, Christopher Laaß, Kathrin Turk, Benjamin E. Iversen, Lars Kotlyarov, Alexey Gaestel, Matthias PLoS One Research Article MK5 (MAPK-activated protein kinase 5) or PRAK (p38-regulated and -activated kinase) are alternative names for a serine/threonine protein kinase downstream to ERK3/4 and p38 MAPK. A previous gene targeting approach for MK5/PRAK (termed here MK5/PRAK-Δex8) revealed a seemingly tumor-suppressive role of MK5/PRAK in DMBA-induced one step skin carcinogenesis and Ras-induced transformation. Here we demonstrate that an alternative targeting strategy of MK5/PRAK (termed MK5/PRAK-Δex6) increased neither tumor incidence in the one step skin carcinogenesis model, nor Ras-induced transformation in primary cells. Interestingly, due to the targeting strategies and exon skipping both knockouts do not completely abolish the generation of MK5/PRAK protein, but express MK5/PRAK deletion mutants with different biochemical properties depending on the exon targeted: Targeting of exon 6 leads to expression of an unstable cytoplasmic catalytically inactive MK5/PRAK-Δex6 mutant while targeting of exon 8 results in a more stable nuclear MK5/PRAK-Δex8 mutant with residual catalytic activity. The different properties of the MK5/PRAK deletion mutants could be responsible for the observed discrepancy between the knockout strains and challenge the role of MK5/PRAK in p53-dependent tumor suppression. Further MK5/PRAK knockout and knock-in mouse strains will be necessary to assign a physiological function to MK5/PRAK in this model organism. Public Library of Science 2015-08-21 /pmc/articles/PMC4546416/ /pubmed/26295581 http://dx.doi.org/10.1371/journal.pone.0136138 Text en © 2015 Ronkina et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ronkina, Natalia
Johansen, Claus
Bohlmann, Lisa
Lafera, Juri
Menon, Manoj B.
Tiedje, Christopher
Laaß, Kathrin
Turk, Benjamin E.
Iversen, Lars
Kotlyarov, Alexey
Gaestel, Matthias
Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title_full Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title_fullStr Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title_full_unstemmed Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title_short Comparative Analysis of Two Gene-Targeting Approaches Challenges the Tumor-Suppressive Role of the Protein Kinase MK5/PRAK
title_sort comparative analysis of two gene-targeting approaches challenges the tumor-suppressive role of the protein kinase mk5/prak
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4546416/
https://www.ncbi.nlm.nih.gov/pubmed/26295581
http://dx.doi.org/10.1371/journal.pone.0136138
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