Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1

BACKGROUND: Over the years, a great deal of effort has been focused on the design and synthesis of potent, linear peptide inhibitors targeting the polo-like kinase 1 (Plk1), which is critically involved in multiple mitotic processes and has been established as an adverse prognostic marker for tumor...

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Autores principales: Murugan, Ravichandran N., Ahn, Mija, Lee, Woo Cheol, Kim, Hye-Yeon, Song, Jung Hyun, Cheong, Chaejoon, Hwang, Eunha, Seo, Ji-Hyung, Shin, Song Yub, Choi, Sun Ho, Park, Jung-Eun, Bang, Jeong Kyu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3819306/
https://www.ncbi.nlm.nih.gov/pubmed/24223211
http://dx.doi.org/10.1371/journal.pone.0080043
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author Murugan, Ravichandran N.
Ahn, Mija
Lee, Woo Cheol
Kim, Hye-Yeon
Song, Jung Hyun
Cheong, Chaejoon
Hwang, Eunha
Seo, Ji-Hyung
Shin, Song Yub
Choi, Sun Ho
Park, Jung-Eun
Bang, Jeong Kyu
author_facet Murugan, Ravichandran N.
Ahn, Mija
Lee, Woo Cheol
Kim, Hye-Yeon
Song, Jung Hyun
Cheong, Chaejoon
Hwang, Eunha
Seo, Ji-Hyung
Shin, Song Yub
Choi, Sun Ho
Park, Jung-Eun
Bang, Jeong Kyu
author_sort Murugan, Ravichandran N.
collection PubMed
description BACKGROUND: Over the years, a great deal of effort has been focused on the design and synthesis of potent, linear peptide inhibitors targeting the polo-like kinase 1 (Plk1), which is critically involved in multiple mitotic processes and has been established as an adverse prognostic marker for tumor patients. Plk1 localizes to its intracellular anchoring sites via its polo-box domain, and inhibiting the Plk1 polo-box domain has been considered as an approach to circumvent the specificity problems associated with inhibiting the conserved adenosine triphosphate-binding pocket. The polo-box domain consists of two different binding regions, such as the unique, broader pyrrolidine-binding pocket and the conserved, narrow, Tyr-rich hydrophobic channel, among the three Plk polo-box domains (Plks 1–3), respectively. Therefore, the studies that provide insights into the binding nature of the unique, broader pyrrolidine-binding pocket might lead to the development of selective Plk1-inhibitory compounds. METHODOLOGY/PRINCIPAL FINDINGS: In an attempt to retain the monospecificity by targeting the unique, broader pyrrolidine-binding pocket, here, for the first time, a systematic approach was undertaken to examine the structure-activity relationship of N-terminal-truncated PLHSpTM derivatives, to apply a site-directed ligand approach using bulky aromatic and non-aromatic systems, and to characterize the binding nature of these analogues using X-ray crystallographic studies. We have identified a new mode of binding interactions, having improved binding affinity and retaining the Plk1 polo-box domain specificity, at the pyrrolidine-binding pocket. Furthermore, our data revealed that the pyrrolidine-binding pocket was very specific to recognize a short and bulky hydrophobic ligand like adamantane, whereas the Tyr-rich hydrophobic channel was specific with lengthy and small hydrophobic groups. CONCLUSION/SIGNIFICANCE: The progress made using our site-directed ligands validated this approach to specifically direct the ligand into the unique pyrrolidine-binding region, and it extends the applicability of the strategy for discovering selective protein-protein interaction inhibitors.
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spelling pubmed-38193062013-11-12 Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1 Murugan, Ravichandran N. Ahn, Mija Lee, Woo Cheol Kim, Hye-Yeon Song, Jung Hyun Cheong, Chaejoon Hwang, Eunha Seo, Ji-Hyung Shin, Song Yub Choi, Sun Ho Park, Jung-Eun Bang, Jeong Kyu PLoS One Research Article BACKGROUND: Over the years, a great deal of effort has been focused on the design and synthesis of potent, linear peptide inhibitors targeting the polo-like kinase 1 (Plk1), which is critically involved in multiple mitotic processes and has been established as an adverse prognostic marker for tumor patients. Plk1 localizes to its intracellular anchoring sites via its polo-box domain, and inhibiting the Plk1 polo-box domain has been considered as an approach to circumvent the specificity problems associated with inhibiting the conserved adenosine triphosphate-binding pocket. The polo-box domain consists of two different binding regions, such as the unique, broader pyrrolidine-binding pocket and the conserved, narrow, Tyr-rich hydrophobic channel, among the three Plk polo-box domains (Plks 1–3), respectively. Therefore, the studies that provide insights into the binding nature of the unique, broader pyrrolidine-binding pocket might lead to the development of selective Plk1-inhibitory compounds. METHODOLOGY/PRINCIPAL FINDINGS: In an attempt to retain the monospecificity by targeting the unique, broader pyrrolidine-binding pocket, here, for the first time, a systematic approach was undertaken to examine the structure-activity relationship of N-terminal-truncated PLHSpTM derivatives, to apply a site-directed ligand approach using bulky aromatic and non-aromatic systems, and to characterize the binding nature of these analogues using X-ray crystallographic studies. We have identified a new mode of binding interactions, having improved binding affinity and retaining the Plk1 polo-box domain specificity, at the pyrrolidine-binding pocket. Furthermore, our data revealed that the pyrrolidine-binding pocket was very specific to recognize a short and bulky hydrophobic ligand like adamantane, whereas the Tyr-rich hydrophobic channel was specific with lengthy and small hydrophobic groups. CONCLUSION/SIGNIFICANCE: The progress made using our site-directed ligands validated this approach to specifically direct the ligand into the unique pyrrolidine-binding region, and it extends the applicability of the strategy for discovering selective protein-protein interaction inhibitors. Public Library of Science 2013-11-06 /pmc/articles/PMC3819306/ /pubmed/24223211 http://dx.doi.org/10.1371/journal.pone.0080043 Text en © 2013 Murugan et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Murugan, Ravichandran N.
Ahn, Mija
Lee, Woo Cheol
Kim, Hye-Yeon
Song, Jung Hyun
Cheong, Chaejoon
Hwang, Eunha
Seo, Ji-Hyung
Shin, Song Yub
Choi, Sun Ho
Park, Jung-Eun
Bang, Jeong Kyu
Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title_full Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title_fullStr Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title_full_unstemmed Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title_short Exploring the Binding Nature of Pyrrolidine Pocket-Dependent Interactions in the Polo-Box Domain of Polo-Like Kinase 1
title_sort exploring the binding nature of pyrrolidine pocket-dependent interactions in the polo-box domain of polo-like kinase 1
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3819306/
https://www.ncbi.nlm.nih.gov/pubmed/24223211
http://dx.doi.org/10.1371/journal.pone.0080043
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