Dynamic changes to survivin subcellular localization are initiated by DNA damage

Maritess Gay Asumen1, Tochukwu V Ifeacho2, Luke Cockerham3, Christina Pfandl4, Nathan R Wall31Touro University’s College of Osteopathic Medicine, Vallejo, CA, USA; 2University of Southern California, Los Angeles, CA, USA; 3Center for Health Disparities Research and Molecular Medicine,...

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Main Authors: Maritess Gay Asumen, Tochukwu V Ifeacho, Luke Cockerham, et al
Format: Article
Language:English
Published: Dove Medical Press 2010-07-01
Series:OncoTargets and Therapy
Online Access:http://www.dovepress.com/dynamic-changes-to-survivin-subcellular-localization-are-initiated-by--a4741
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spelling doaj-d0ff47d10e1945768ac712d9bb65aed72020-11-25T00:34:43ZengDove Medical PressOncoTargets and Therapy1178-69302010-07-012010default129137Dynamic changes to survivin subcellular localization are initiated by DNA damageMaritess Gay AsumenTochukwu V IfeachoLuke Cockerhamet alMaritess Gay Asumen1, Tochukwu V Ifeacho2, Luke Cockerham3, Christina Pfandl4, Nathan R Wall31Touro University’s College of Osteopathic Medicine, Vallejo, CA, USA; 2University of Southern California, Los Angeles, CA, USA; 3Center for Health Disparities Research and Molecular Medicine, Loma Linda University, CA, USA; 4Green Mountain Antibodies, Burlington, VT, USAAbstract: Subcellular distribution of the apoptosis inhibitor survivin and its ability to relocalize as a result of cell cycle phase or therapeutic insult has led to the hypothesis that these subcellular pools may coincide with different survivin functions. The PIK kinases (ATM, ATR and DNA-PK) phosphorylate a variety of effector substrates that propagate DNA damage signals, resulting in various biological outputs. Here we demonstrate that subcellular repartitioning of survivin in MCF-7 cells as a result of UV light-mediated DNA damage is dependent upon DNA damage-sensing proteins as treatment with the pan PIK kinase inhibitor wortmannin repartitioned survivin in the mitochondria and diminished it from the cytosol and nucleus. Mitochondrial redistribution of survivin, such as was recorded after wortmannin treatment, occurred in cells lacking any one of the three DNA damage sensing protein kinases: DNA-PK, ATM or ATR. However, failed survivin redistribution from the mitochondria in response to low-dose UV occurred only in the cells lacking ATM, implying that ATM may be the primary kinase involved in this process. Taken together, this data implicates survivian’s subcellular distribution is a dynamic physiological process that appears responsive to UV light- initiated DNA damage and that its distribution may be responsible for its multifunctionality.Keywords: survivin, PIK kinases, ATM, ATR, DNA-PK http://www.dovepress.com/dynamic-changes-to-survivin-subcellular-localization-are-initiated-by--a4741
collection DOAJ
language English
format Article
sources DOAJ
author Maritess Gay Asumen
Tochukwu V Ifeacho
Luke Cockerham
et al
spellingShingle Maritess Gay Asumen
Tochukwu V Ifeacho
Luke Cockerham
et al
Dynamic changes to survivin subcellular localization are initiated by DNA damage
OncoTargets and Therapy
author_facet Maritess Gay Asumen
Tochukwu V Ifeacho
Luke Cockerham
et al
author_sort Maritess Gay Asumen
title Dynamic changes to survivin subcellular localization are initiated by DNA damage
title_short Dynamic changes to survivin subcellular localization are initiated by DNA damage
title_full Dynamic changes to survivin subcellular localization are initiated by DNA damage
title_fullStr Dynamic changes to survivin subcellular localization are initiated by DNA damage
title_full_unstemmed Dynamic changes to survivin subcellular localization are initiated by DNA damage
title_sort dynamic changes to survivin subcellular localization are initiated by dna damage
publisher Dove Medical Press
series OncoTargets and Therapy
issn 1178-6930
publishDate 2010-07-01
description Maritess Gay Asumen1, Tochukwu V Ifeacho2, Luke Cockerham3, Christina Pfandl4, Nathan R Wall31Touro University’s College of Osteopathic Medicine, Vallejo, CA, USA; 2University of Southern California, Los Angeles, CA, USA; 3Center for Health Disparities Research and Molecular Medicine, Loma Linda University, CA, USA; 4Green Mountain Antibodies, Burlington, VT, USAAbstract: Subcellular distribution of the apoptosis inhibitor survivin and its ability to relocalize as a result of cell cycle phase or therapeutic insult has led to the hypothesis that these subcellular pools may coincide with different survivin functions. The PIK kinases (ATM, ATR and DNA-PK) phosphorylate a variety of effector substrates that propagate DNA damage signals, resulting in various biological outputs. Here we demonstrate that subcellular repartitioning of survivin in MCF-7 cells as a result of UV light-mediated DNA damage is dependent upon DNA damage-sensing proteins as treatment with the pan PIK kinase inhibitor wortmannin repartitioned survivin in the mitochondria and diminished it from the cytosol and nucleus. Mitochondrial redistribution of survivin, such as was recorded after wortmannin treatment, occurred in cells lacking any one of the three DNA damage sensing protein kinases: DNA-PK, ATM or ATR. However, failed survivin redistribution from the mitochondria in response to low-dose UV occurred only in the cells lacking ATM, implying that ATM may be the primary kinase involved in this process. Taken together, this data implicates survivian’s subcellular distribution is a dynamic physiological process that appears responsive to UV light- initiated DNA damage and that its distribution may be responsible for its multifunctionality.Keywords: survivin, PIK kinases, ATM, ATR, DNA-PK
url http://www.dovepress.com/dynamic-changes-to-survivin-subcellular-localization-are-initiated-by--a4741
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