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Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function

Plant homeodomain fingers (PHD-fingers) are a family of reader domains that can recruit epigenetic proteins to specific histone modification sites. Many PHD-fingers recognise methylated lysines on histone tails and play crucial roles in transcriptional regulation, with their dysregulation linked to...

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Autores principales: Coleman, Oliver D., Macdonald, Jessica, Thomson, Ben, Ward, Jennifer A., Stubbs, Christopher J., McAllister, Tom E., Clark, Shane, Amin, Siddique, Cao, Yimang, Abboud, Martine I., Zhang, Yijia, Sanganee, Hitesh, Huber, Kilian V. M., Claridge, Tim D. W., Kawamura, Akane
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10321576/
https://www.ncbi.nlm.nih.gov/pubmed/37416723
http://dx.doi.org/10.1039/d2sc05944d
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author Coleman, Oliver D.
Macdonald, Jessica
Thomson, Ben
Ward, Jennifer A.
Stubbs, Christopher J.
McAllister, Tom E.
Clark, Shane
Amin, Siddique
Cao, Yimang
Abboud, Martine I.
Zhang, Yijia
Sanganee, Hitesh
Huber, Kilian V. M.
Claridge, Tim D. W.
Kawamura, Akane
author_facet Coleman, Oliver D.
Macdonald, Jessica
Thomson, Ben
Ward, Jennifer A.
Stubbs, Christopher J.
McAllister, Tom E.
Clark, Shane
Amin, Siddique
Cao, Yimang
Abboud, Martine I.
Zhang, Yijia
Sanganee, Hitesh
Huber, Kilian V. M.
Claridge, Tim D. W.
Kawamura, Akane
author_sort Coleman, Oliver D.
collection PubMed
description Plant homeodomain fingers (PHD-fingers) are a family of reader domains that can recruit epigenetic proteins to specific histone modification sites. Many PHD-fingers recognise methylated lysines on histone tails and play crucial roles in transcriptional regulation, with their dysregulation linked to various human diseases. Despite their biological importance, chemical inhibitors for targeting PHD-fingers are very limited. Here we report a potent and selective de novo cyclic peptide inhibitor (OC9) targeting the N(ε)-trimethyllysine-binding PHD-fingers of the KDM7 histone demethylases, developed using mRNA display. OC9 disrupts PHD-finger interaction with histone H3K4me3 by engaging the N(ε)-methyllysine-binding aromatic cage through a valine, revealing a new non-lysine recognition motif for the PHD-fingers that does not require cation-π interaction. PHD-finger inhibition by OC9 impacted JmjC-domain mediated demethylase activity at H3K9me2, leading to inhibition of KDM7B (PHF8) but stimulation of KDM7A (KIAA1718), representing a new approach for selective allosteric modulation of demethylase activity. Chemoproteomic analysis showed selective engagement of OC9 with KDM7s in T cell lymphoblastic lymphoma SUP T1 cells. Our results highlight the utility of mRNA-display derived cyclic peptides for targeting challenging epigenetic reader proteins to probe their biology, and the broader potential of this approach for targeting protein–protein interactions.
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spelling pubmed-103215762023-07-06 Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function Coleman, Oliver D. Macdonald, Jessica Thomson, Ben Ward, Jennifer A. Stubbs, Christopher J. McAllister, Tom E. Clark, Shane Amin, Siddique Cao, Yimang Abboud, Martine I. Zhang, Yijia Sanganee, Hitesh Huber, Kilian V. M. Claridge, Tim D. W. Kawamura, Akane Chem Sci Chemistry Plant homeodomain fingers (PHD-fingers) are a family of reader domains that can recruit epigenetic proteins to specific histone modification sites. Many PHD-fingers recognise methylated lysines on histone tails and play crucial roles in transcriptional regulation, with their dysregulation linked to various human diseases. Despite their biological importance, chemical inhibitors for targeting PHD-fingers are very limited. Here we report a potent and selective de novo cyclic peptide inhibitor (OC9) targeting the N(ε)-trimethyllysine-binding PHD-fingers of the KDM7 histone demethylases, developed using mRNA display. OC9 disrupts PHD-finger interaction with histone H3K4me3 by engaging the N(ε)-methyllysine-binding aromatic cage through a valine, revealing a new non-lysine recognition motif for the PHD-fingers that does not require cation-π interaction. PHD-finger inhibition by OC9 impacted JmjC-domain mediated demethylase activity at H3K9me2, leading to inhibition of KDM7B (PHF8) but stimulation of KDM7A (KIAA1718), representing a new approach for selective allosteric modulation of demethylase activity. Chemoproteomic analysis showed selective engagement of OC9 with KDM7s in T cell lymphoblastic lymphoma SUP T1 cells. Our results highlight the utility of mRNA-display derived cyclic peptides for targeting challenging epigenetic reader proteins to probe their biology, and the broader potential of this approach for targeting protein–protein interactions. The Royal Society of Chemistry 2023-04-17 /pmc/articles/PMC10321576/ /pubmed/37416723 http://dx.doi.org/10.1039/d2sc05944d Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by/3.0/
spellingShingle Chemistry
Coleman, Oliver D.
Macdonald, Jessica
Thomson, Ben
Ward, Jennifer A.
Stubbs, Christopher J.
McAllister, Tom E.
Clark, Shane
Amin, Siddique
Cao, Yimang
Abboud, Martine I.
Zhang, Yijia
Sanganee, Hitesh
Huber, Kilian V. M.
Claridge, Tim D. W.
Kawamura, Akane
Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title_full Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title_fullStr Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title_full_unstemmed Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title_short Cyclic peptides target the aromatic cage of a PHD-finger reader domain to modulate epigenetic protein function
title_sort cyclic peptides target the aromatic cage of a phd-finger reader domain to modulate epigenetic protein function
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10321576/
https://www.ncbi.nlm.nih.gov/pubmed/37416723
http://dx.doi.org/10.1039/d2sc05944d
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