Reversible inactivation of the transcriptional function of P53 protein by farnesylation

Reversible inactivation of the transcriptional function of P53 protein by farnesylation

<p>Abstract</p> <p>Background</p> <p>The use of integrating viral vectors in Gene therapy clinical trials has pointed out the problem of the deleterous effect of the integration of the ectopic gene to the cellular genome and the safety of this strategy. We proposed here...

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Main Authors: Berg Danièle, Casteignau Antoine, Pradines Anne, Tohfe Mustapha, Penary Marie, Couderc Bettina, Favre Gilles
Format: Article
Language:English
Published: BMC 2006-05-01
Series:BMC Biotechnology
Online Access:http://www.biomedcentral.com/1472-6750/6/26
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spelling doaj-a03bc3d7dd1a4868a23225acf1da4ae32020-11-25T03:37:34ZengBMCBMC Biotechnology1472-67502006-05-01612610.1186/1472-6750-6-26Reversible inactivation of the transcriptional function of P53 protein by farnesylationBerg DanièleCasteignau AntoinePradines AnneTohfe MustaphaPenary MarieCouderc BettinaFavre Gilles<p>Abstract</p> <p>Background</p> <p>The use of integrating viral vectors in Gene therapy clinical trials has pointed out the problem of the deleterous effect of the integration of the ectopic gene to the cellular genome and the safety of this strategy. We proposed here a way to induce the death of gene modified cells upon request by acting on a pro-apoptotic protein cellular localization and on the activation of its apoptotic function.</p> <p>Results</p> <p>We constructed an adenoviral vector coding a chimeric p53 protein by fusing p53 sequence with the 21 COOH term amino acids sequence of H-Ras. Indeed, the translation products of Ras genes are cytosolic proteins that become secondarily associated with membranes through a series of post-translational modifications initiated by a CAAX motif present at the C terminus of Ras proteins. The chimeric p53HRCaax protein was farnesylated efficiently in transduced human osteosarcoma p53-/- cell line. The farnesylated form of p53 resided mainly in the cytosol, where it is non-functional. Farnesyl transferase inhibitors (FTIs) specifically inhibited farnesyl isoprenoid lipid modification of proteins. Following treatment of the cells with an FTI, p53HRCaax underwent translocation into the nucleus where it retained transcription factor activity. Shifting p53 into the nucleus resulted in the induction of p21<sup>waf1/CIP1 </sup>and Bax transcription, cell growth arrest, caspase activation and apoptosis.</p> <p>Conclusion</p> <p>Artificial protein farnesylation impaired the transcriptional activity of p53. This could be prevented by Farnesyl transferase inhibition. These data highlight the fact that the artificial prenylation of proteins provides a novel system for controlling the function of a transactivating factor.</p> http://www.biomedcentral.com/1472-6750/6/26
collection DOAJ
language English
format Article
sources DOAJ
author Berg Danièle
Casteignau Antoine
Pradines Anne
Tohfe Mustapha
Penary Marie
Couderc Bettina
Favre Gilles
spellingShingle Berg Danièle
Casteignau Antoine
Pradines Anne
Tohfe Mustapha
Penary Marie
Couderc Bettina
Favre Gilles
Reversible inactivation of the transcriptional function of P53 protein by farnesylation
BMC Biotechnology
author_facet Berg Danièle
Casteignau Antoine
Pradines Anne
Tohfe Mustapha
Penary Marie
Couderc Bettina
Favre Gilles
author_sort Berg Danièle
title Reversible inactivation of the transcriptional function of P53 protein by farnesylation
title_short Reversible inactivation of the transcriptional function of P53 protein by farnesylation
title_full Reversible inactivation of the transcriptional function of P53 protein by farnesylation
title_fullStr Reversible inactivation of the transcriptional function of P53 protein by farnesylation
title_full_unstemmed Reversible inactivation of the transcriptional function of P53 protein by farnesylation
title_sort reversible inactivation of the transcriptional function of p53 protein by farnesylation
publisher BMC
series BMC Biotechnology
issn 1472-6750
publishDate 2006-05-01
description <p>Abstract</p> <p>Background</p> <p>The use of integrating viral vectors in Gene therapy clinical trials has pointed out the problem of the deleterous effect of the integration of the ectopic gene to the cellular genome and the safety of this strategy. We proposed here a way to induce the death of gene modified cells upon request by acting on a pro-apoptotic protein cellular localization and on the activation of its apoptotic function.</p> <p>Results</p> <p>We constructed an adenoviral vector coding a chimeric p53 protein by fusing p53 sequence with the 21 COOH term amino acids sequence of H-Ras. Indeed, the translation products of Ras genes are cytosolic proteins that become secondarily associated with membranes through a series of post-translational modifications initiated by a CAAX motif present at the C terminus of Ras proteins. The chimeric p53HRCaax protein was farnesylated efficiently in transduced human osteosarcoma p53-/- cell line. The farnesylated form of p53 resided mainly in the cytosol, where it is non-functional. Farnesyl transferase inhibitors (FTIs) specifically inhibited farnesyl isoprenoid lipid modification of proteins. Following treatment of the cells with an FTI, p53HRCaax underwent translocation into the nucleus where it retained transcription factor activity. Shifting p53 into the nucleus resulted in the induction of p21<sup>waf1/CIP1 </sup>and Bax transcription, cell growth arrest, caspase activation and apoptosis.</p> <p>Conclusion</p> <p>Artificial protein farnesylation impaired the transcriptional activity of p53. This could be prevented by Farnesyl transferase inhibition. These data highlight the fact that the artificial prenylation of proteins provides a novel system for controlling the function of a transactivating factor.</p>
url http://www.biomedcentral.com/1472-6750/6/26
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AT pradinesanne reversibleinactivationofthetranscriptionalfunctionofp53proteinbyfarnesylation
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AT penarymarie reversibleinactivationofthetranscriptionalfunctionofp53proteinbyfarnesylation
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