Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor

BACKGROUND: Structure-based drug design (SBDD) can accelerate inhibitor lead design and optimization, and efficient methods including protein purification, characterization, crystallization, and high-resolution diffraction are all needed for rapid, iterative structure determination. Janus kinases ar...

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Autores principales: Argiriadi, Maria A, Goedken, Eric R, Banach, David, Borhani, David W, Burchat, Andrew, Dixon, Richard W, Marcotte, Doug, Overmeyer, Gary, Pivorunas, Valerie, Sadhukhan, Ramkrishna, Sousa, Silvino, Moore, Nigel St John, Tomlinson, Medha, Voss, Jeffrey, Wang, Lu, Wishart, Neil, Woller, Kevin, Talanian, Robert V
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3478977/
https://www.ncbi.nlm.nih.gov/pubmed/22995073
http://dx.doi.org/10.1186/1472-6807-12-22
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author Argiriadi, Maria A
Goedken, Eric R
Banach, David
Borhani, David W
Burchat, Andrew
Dixon, Richard W
Marcotte, Doug
Overmeyer, Gary
Pivorunas, Valerie
Sadhukhan, Ramkrishna
Sousa, Silvino
Moore, Nigel St John
Tomlinson, Medha
Voss, Jeffrey
Wang, Lu
Wishart, Neil
Woller, Kevin
Talanian, Robert V
author_facet Argiriadi, Maria A
Goedken, Eric R
Banach, David
Borhani, David W
Burchat, Andrew
Dixon, Richard W
Marcotte, Doug
Overmeyer, Gary
Pivorunas, Valerie
Sadhukhan, Ramkrishna
Sousa, Silvino
Moore, Nigel St John
Tomlinson, Medha
Voss, Jeffrey
Wang, Lu
Wishart, Neil
Woller, Kevin
Talanian, Robert V
author_sort Argiriadi, Maria A
collection PubMed
description BACKGROUND: Structure-based drug design (SBDD) can accelerate inhibitor lead design and optimization, and efficient methods including protein purification, characterization, crystallization, and high-resolution diffraction are all needed for rapid, iterative structure determination. Janus kinases are important targets that are amenable to structure-based drug design. Here we present the first mouse Tyk2 crystal structures, which are complexed to 3-aminoindazole compounds. RESULTS: A comprehensive construct design effort included N- and C-terminal variations, kinase-inactive mutations, and multiple species orthologs. High-throughput cloning and expression methods were coupled with an abbreviated purification protocol to optimize protein solubility and stability. In total, 50 Tyk2 constructs were generated. Many displayed poor expression, inadequate solubility, or incomplete affinity tag processing. One kinase-inactive murine Tyk2 construct, complexed with an ATP-competitive 3-aminoindazole inhibitor, provided crystals that diffracted to 2.5–2.6 Å resolution. This structure revealed initial “hot-spot” regions for SBDD, and provided a robust platform for ligand soaking experiments. Compared to previously reported human Tyk2 inhibitor crystal structures (Chrencik et al. (2010) J Mol Biol 400:413), our structures revealed a key difference in the glycine-rich loop conformation that is induced by the inhibitor. Ligand binding also conferred resistance to proteolytic degradation by thermolysin. As crystals could not be obtained with the unliganded enzyme, this enhanced stability is likely important for successful crystallization and inhibitor soaking methods. CONCLUSIONS: Practical criteria for construct performance and prioritization, the optimization of purification protocols to enhance protein yields and stability, and use of high-throughput construct exploration enable structure determination methods early in the drug discovery process. Additionally, specific ligands stabilize Tyk2 protein and may thereby enable crystallization.
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spelling pubmed-34789772012-10-24 Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor Argiriadi, Maria A Goedken, Eric R Banach, David Borhani, David W Burchat, Andrew Dixon, Richard W Marcotte, Doug Overmeyer, Gary Pivorunas, Valerie Sadhukhan, Ramkrishna Sousa, Silvino Moore, Nigel St John Tomlinson, Medha Voss, Jeffrey Wang, Lu Wishart, Neil Woller, Kevin Talanian, Robert V BMC Struct Biol Research Article BACKGROUND: Structure-based drug design (SBDD) can accelerate inhibitor lead design and optimization, and efficient methods including protein purification, characterization, crystallization, and high-resolution diffraction are all needed for rapid, iterative structure determination. Janus kinases are important targets that are amenable to structure-based drug design. Here we present the first mouse Tyk2 crystal structures, which are complexed to 3-aminoindazole compounds. RESULTS: A comprehensive construct design effort included N- and C-terminal variations, kinase-inactive mutations, and multiple species orthologs. High-throughput cloning and expression methods were coupled with an abbreviated purification protocol to optimize protein solubility and stability. In total, 50 Tyk2 constructs were generated. Many displayed poor expression, inadequate solubility, or incomplete affinity tag processing. One kinase-inactive murine Tyk2 construct, complexed with an ATP-competitive 3-aminoindazole inhibitor, provided crystals that diffracted to 2.5–2.6 Å resolution. This structure revealed initial “hot-spot” regions for SBDD, and provided a robust platform for ligand soaking experiments. Compared to previously reported human Tyk2 inhibitor crystal structures (Chrencik et al. (2010) J Mol Biol 400:413), our structures revealed a key difference in the glycine-rich loop conformation that is induced by the inhibitor. Ligand binding also conferred resistance to proteolytic degradation by thermolysin. As crystals could not be obtained with the unliganded enzyme, this enhanced stability is likely important for successful crystallization and inhibitor soaking methods. CONCLUSIONS: Practical criteria for construct performance and prioritization, the optimization of purification protocols to enhance protein yields and stability, and use of high-throughput construct exploration enable structure determination methods early in the drug discovery process. Additionally, specific ligands stabilize Tyk2 protein and may thereby enable crystallization. BioMed Central 2012-09-20 /pmc/articles/PMC3478977/ /pubmed/22995073 http://dx.doi.org/10.1186/1472-6807-12-22 Text en Copyright ©2012 Argiriadi et al.; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Argiriadi, Maria A
Goedken, Eric R
Banach, David
Borhani, David W
Burchat, Andrew
Dixon, Richard W
Marcotte, Doug
Overmeyer, Gary
Pivorunas, Valerie
Sadhukhan, Ramkrishna
Sousa, Silvino
Moore, Nigel St John
Tomlinson, Medha
Voss, Jeffrey
Wang, Lu
Wishart, Neil
Woller, Kevin
Talanian, Robert V
Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title_full Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title_fullStr Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title_full_unstemmed Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title_short Enabling structure-based drug design of Tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
title_sort enabling structure-based drug design of tyk2 through co-crystallization with a stabilizing aminoindazole inhibitor
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3478977/
https://www.ncbi.nlm.nih.gov/pubmed/22995073
http://dx.doi.org/10.1186/1472-6807-12-22
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