DocumentCode :
1392818
Title :
Sensitivity analysis predicts that the ERK-pMEK interaction regulates ERK
Author :
Radhakrishnan, Krishnaja ; Edwards, Jeremy S. ; Lidke, D.S. ; Jovin, T.M. ; Wilson, B.S. ; Oliver, J. Marcus
Author_Institution :
Sch. of Med., Dept. of Pathology, Univ. of New Mexico, Albuquerque, NM, USA
Volume :
3
Issue :
5
fYear :
2009
fDate :
9/1/2009 12:00:00 AM
Firstpage :
329
Lastpage :
341
Abstract :
Following phosphorylation, nuclear translocation of the mitogen-activated protein kinases (MAPKs), ERK1 and ERK2, is critical for both gene expression and DNA replication induced by growth factors. ERK nuclear translocation has therefore been studied extensively, but many details remain unresolved, including whether or not ERK dimerisation is required for translocation. Here, we simulate ERK nuclear translocation with a compartmental computational model that includes systematic sensitivity analysis. The governing ordinary differential equations are solved with the backward differentiation formula and decoupled direct methods. To better understand the regulation of ERK nuclear translocation, we use this model in conjunction with a previously published model of the ERK pathway that does not include an ERK dimer species and with experimental measurements of nuclear translocation of wild-type ERK and a mutant form, ERK1-Delta4, which is unable to dimerise. Sensitivity analysis reveals that the delayed nuclear uptake of ERK1-Delta4 compared to that of wild-type ERK1 can be explained by the altered interaction of ERK1-Delta4 with phosphorylated MEK (MAPK/ERK kinase), and so may be independent of dimerisation. Our study also identifies biological experiments that can verify this explanation.
Keywords :
DNA; biochemistry; cellular biophysics; differential equations; genetics; molecular biophysics; proteins; sensitivity analysis; DNA replication; ERK dimer species; ERK dimerisation; ERK nuclear translocation; ERK-pMEK interaction regulation; ERK1; ERK2; delayed nuclear uptake; extracellular signal-regulated kinase 1; extracellular signal-regulated kinase 2; gene expression; mitogen-activated protein kinases; ordinary differential equations; phosphorylation; sensitivity analysis prediction; systematic sensitivity analysis; wild-type ERK pathway;
fLanguage :
English
Journal_Title :
Systems Biology, IET
Publisher :
iet
ISSN :
1751-8849
Type :
jour
DOI :
10.1049/iet-syb.2009.0010
Filename :
5243211
Link To Document :
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