Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.

Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.

Mutated tyrosine kinases are associated with a number of different haematological malignancies including myeloproliferative disorders, lymphoma and acute myeloid leukaemia. The potential commonalities in the action of six of these leukemogenic proteins on nuclear proteins were investigated using sys...

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Autores principales: Andrew Pierce, Andrew Williamson, Ewa Jaworska, John R Griffiths, Sam Taylor, Michael Walker, Mark Aspinall-O'Dea, Elaine Spooncer, Richard D Unwin, Toryn Poolman, David Ray, Anthony D Whetton
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Publicado: Public Library of Science (PLoS) 2012
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spelling oai:doaj.org-article:196965d7fc1a435eaf81238cb16e88182021-11-18T07:14:41ZIdentification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.1932-620310.1371/journal.pone.0038928https://doaj.org/article/196965d7fc1a435eaf81238cb16e88182012-01-01T00:00:00Zhttps://www.ncbi.nlm.nih.gov/pmc/articles/pmid/22745689/pdf/?tool=EBIhttps://doaj.org/toc/1932-6203Mutated tyrosine kinases are associated with a number of different haematological malignancies including myeloproliferative disorders, lymphoma and acute myeloid leukaemia. The potential commonalities in the action of six of these leukemogenic proteins on nuclear proteins were investigated using systematic proteomic analysis. The effects on over 3600 nuclear proteins and 1500 phosphopeptide sites were relatively quantified in seven isogenic cell lines. The effects of the kinases were diverse although some commonalities were found. Comparison of the nuclear proteomic data with transcriptome data and cytoplasmic proteomic data indicated that the major changes are due to post-translational mechanisms rather than changes in mRNA or protein distribution. Analysis of the promoter regions of genes whose protein levels changed in response to the kinases showed the most common binding site found was that for NFκB whilst other sites such as those for the glucocorticoid receptor were also found. Glucocorticoid receptor levels and phosphorylation were decreased by all 6 PTKs. Whilst Glucocorticoid receptor action can potentiate NFκB action those proteins where genes have NFκB binding sites were in often regulated post-translationally. However all 6 PTKs showed evidence of NFkB pathway modulation via activation via altered IkB and NFKB levels. Validation of a common change was also undertaken with PMS2, a DNA mismatch repair protein. PMS2 nuclear levels were decreased in response to the expression of all 6 kinases, with no concomitant change in mRNA level or cytosolic protein level. Response to thioguanine, that requires the mismatch repair pathway, was modulated by all 6 oncogenic kinases. In summary common targets for 6 oncogenic PTKs have been found that are regulated by post-translational mechanisms. They represent potential new avenues for therapies but also demonstrate the post-translational regulation is a key target of leukaemogenic kinases.Andrew PierceAndrew WilliamsonEwa JaworskaJohn R GriffithsSam TaylorMichael WalkerMark Aspinall-O'DeaElaine SpooncerRichard D UnwinToryn PoolmanDavid RayAnthony D WhettonPublic Library of Science (PLoS)articleMedicineRScienceQENPLoS ONE, Vol 7, Iss 6, p e38928 (2012)
institution DOAJ
collection DOAJ
language EN
topic Medicine
R
Science
Q
spellingShingle Medicine
R
Science
Q
Andrew Pierce
Andrew Williamson
Ewa Jaworska
John R Griffiths
Sam Taylor
Michael Walker
Mark Aspinall-O'Dea
Elaine Spooncer
Richard D Unwin
Toryn Poolman
David Ray
Anthony D Whetton
Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
description Mutated tyrosine kinases are associated with a number of different haematological malignancies including myeloproliferative disorders, lymphoma and acute myeloid leukaemia. The potential commonalities in the action of six of these leukemogenic proteins on nuclear proteins were investigated using systematic proteomic analysis. The effects on over 3600 nuclear proteins and 1500 phosphopeptide sites were relatively quantified in seven isogenic cell lines. The effects of the kinases were diverse although some commonalities were found. Comparison of the nuclear proteomic data with transcriptome data and cytoplasmic proteomic data indicated that the major changes are due to post-translational mechanisms rather than changes in mRNA or protein distribution. Analysis of the promoter regions of genes whose protein levels changed in response to the kinases showed the most common binding site found was that for NFκB whilst other sites such as those for the glucocorticoid receptor were also found. Glucocorticoid receptor levels and phosphorylation were decreased by all 6 PTKs. Whilst Glucocorticoid receptor action can potentiate NFκB action those proteins where genes have NFκB binding sites were in often regulated post-translationally. However all 6 PTKs showed evidence of NFkB pathway modulation via activation via altered IkB and NFKB levels. Validation of a common change was also undertaken with PMS2, a DNA mismatch repair protein. PMS2 nuclear levels were decreased in response to the expression of all 6 kinases, with no concomitant change in mRNA level or cytosolic protein level. Response to thioguanine, that requires the mismatch repair pathway, was modulated by all 6 oncogenic kinases. In summary common targets for 6 oncogenic PTKs have been found that are regulated by post-translational mechanisms. They represent potential new avenues for therapies but also demonstrate the post-translational regulation is a key target of leukaemogenic kinases.
format article
author Andrew Pierce
Andrew Williamson
Ewa Jaworska
John R Griffiths
Sam Taylor
Michael Walker
Mark Aspinall-O'Dea
Elaine Spooncer
Richard D Unwin
Toryn Poolman
David Ray
Anthony D Whetton
author_facet Andrew Pierce
Andrew Williamson
Ewa Jaworska
John R Griffiths
Sam Taylor
Michael Walker
Mark Aspinall-O'Dea
Elaine Spooncer
Richard D Unwin
Toryn Poolman
David Ray
Anthony D Whetton
author_sort Andrew Pierce
title Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
title_short Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
title_full Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
title_fullStr Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
title_full_unstemmed Identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
title_sort identification of nuclear protein targets for six leukemogenic tyrosine kinases governed by post-translational regulation.
publisher Public Library of Science (PLoS)
publishDate 2012
url https://doaj.org/article/196965d7fc1a435eaf81238cb16e8818
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