Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1

Ligands that can selectively bind to proteins with single amino acid point mutations offer the potential to detect or treat an abnormal protein in the presence of the wildtype. However, it is difficult to develop a selective ligand if the point mutation is not associated with an addressable location...

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Autores principales: Deyle, Kaycie M., Farrow, Blake, Hee, Ying Qiao, Work, Jeremy, Wong, Michelle, Lai, Bert, Umeda, Aiko, Millward, Steven W., Nag, Arundhati, Das, Samir, Heath, James R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2015
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4408887/
https://www.ncbi.nlm.nih.gov/pubmed/25901825
http://dx.doi.org/10.1038/nchem.2223
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author Deyle, Kaycie M.
Farrow, Blake
Hee, Ying Qiao
Work, Jeremy
Wong, Michelle
Lai, Bert
Umeda, Aiko
Millward, Steven W.
Nag, Arundhati
Das, Samir
Heath, James R.
author_facet Deyle, Kaycie M.
Farrow, Blake
Hee, Ying Qiao
Work, Jeremy
Wong, Michelle
Lai, Bert
Umeda, Aiko
Millward, Steven W.
Nag, Arundhati
Das, Samir
Heath, James R.
author_sort Deyle, Kaycie M.
collection PubMed
description Ligands that can selectively bind to proteins with single amino acid point mutations offer the potential to detect or treat an abnormal protein in the presence of the wildtype. However, it is difficult to develop a selective ligand if the point mutation is not associated with an addressable location, such as a binding pocket. Here we report an all-chemical, synthetic epitope-targeting strategy which we used to discover a 5-mer peptide with selectivity for the E17K transforming point mutation in the Pleckstrin Homology Domain of the Akt1 oncoprotein. A fragment of Akt1 containing the E17K mutation and a I19[Propargylglycine] substitution was synthesized to form an addressable synthetic epitope. Azide-presenting peptides that covalently clicked onto this alkyne-presenting epitope were selected from a library using in situ screening. One peptide exhibits a 10:1 in vitro selectivity for the oncoprotein relative to wildtype, with a similar selectivity in cells. This 5-mer peptide was expanded into a larger ligand that selectively blocks the E17K Akt1 interaction with its PIP3 substrate.
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spelling pubmed-44088872015-11-01 Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1 Deyle, Kaycie M. Farrow, Blake Hee, Ying Qiao Work, Jeremy Wong, Michelle Lai, Bert Umeda, Aiko Millward, Steven W. Nag, Arundhati Das, Samir Heath, James R. Nat Chem Article Ligands that can selectively bind to proteins with single amino acid point mutations offer the potential to detect or treat an abnormal protein in the presence of the wildtype. However, it is difficult to develop a selective ligand if the point mutation is not associated with an addressable location, such as a binding pocket. Here we report an all-chemical, synthetic epitope-targeting strategy which we used to discover a 5-mer peptide with selectivity for the E17K transforming point mutation in the Pleckstrin Homology Domain of the Akt1 oncoprotein. A fragment of Akt1 containing the E17K mutation and a I19[Propargylglycine] substitution was synthesized to form an addressable synthetic epitope. Azide-presenting peptides that covalently clicked onto this alkyne-presenting epitope were selected from a library using in situ screening. One peptide exhibits a 10:1 in vitro selectivity for the oncoprotein relative to wildtype, with a similar selectivity in cells. This 5-mer peptide was expanded into a larger ligand that selectively blocks the E17K Akt1 interaction with its PIP3 substrate. 2015-04-13 2015-05 /pmc/articles/PMC4408887/ /pubmed/25901825 http://dx.doi.org/10.1038/nchem.2223 Text en http://www.nature.com/authors/editorial_policies/license.html#terms Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use:http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Deyle, Kaycie M.
Farrow, Blake
Hee, Ying Qiao
Work, Jeremy
Wong, Michelle
Lai, Bert
Umeda, Aiko
Millward, Steven W.
Nag, Arundhati
Das, Samir
Heath, James R.
Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title_full Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title_fullStr Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title_full_unstemmed Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title_short Protein-targeting strategy used to develop a selective inhibitor of the E17K point mutation in the PH Domain of Akt1
title_sort protein-targeting strategy used to develop a selective inhibitor of the e17k point mutation in the ph domain of akt1
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4408887/
https://www.ncbi.nlm.nih.gov/pubmed/25901825
http://dx.doi.org/10.1038/nchem.2223
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