Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry

[Image: see text] Tuberculosis is a major global public health concern, and new drugs are needed to combat both the typical form and the increasingly common drug-resistant form of this disease. The essential tuberculosis kinase PknB is an attractive drug development target because of its central imp...

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Autores principales: Wlodarchak, Nathan, Feltenberger, John B., Ye, Zhengqing, Beczkiewicz, Jeffrey, Procknow, Rebecca, Yan, Gang, King, Troy M., Golden, Jennifer E., Striker, Rob
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2021
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8757511/
https://www.ncbi.nlm.nih.gov/pubmed/35035774
http://dx.doi.org/10.1021/acsmedchemlett.0c00580
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author Wlodarchak, Nathan
Feltenberger, John B.
Ye, Zhengqing
Beczkiewicz, Jeffrey
Procknow, Rebecca
Yan, Gang
King, Troy M.
Golden, Jennifer E.
Striker, Rob
author_facet Wlodarchak, Nathan
Feltenberger, John B.
Ye, Zhengqing
Beczkiewicz, Jeffrey
Procknow, Rebecca
Yan, Gang
King, Troy M.
Golden, Jennifer E.
Striker, Rob
author_sort Wlodarchak, Nathan
collection PubMed
description [Image: see text] Tuberculosis is a major global public health concern, and new drugs are needed to combat both the typical form and the increasingly common drug-resistant form of this disease. The essential tuberculosis kinase PknB is an attractive drug development target because of its central importance in several critical signaling cascades. A major hurdle in kinase inhibitor development is the reduction of toxicity due to nonspecific kinase activity in host cells. Here a novel class of PknB inhibitors was developed from hit aminopyrimidine 1 (GW779439X), which was originally designed for human CDK4 but failed to progress clinically because of high toxicity and low specificity. Replacing the pyrazolopyridazine headgroup of the original hit with substituted pyridine or phenyl headgroups resulted in a reduction of Cdk activity and a 3-fold improvement in specificity over the human kinome while maintaining PknB activity. This also resulted in improved microbiological activity and reduced toxicity in THP-1 cells and zebrafish.
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spelling pubmed-87575112022-01-14 Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry Wlodarchak, Nathan Feltenberger, John B. Ye, Zhengqing Beczkiewicz, Jeffrey Procknow, Rebecca Yan, Gang King, Troy M. Golden, Jennifer E. Striker, Rob ACS Med Chem Lett [Image: see text] Tuberculosis is a major global public health concern, and new drugs are needed to combat both the typical form and the increasingly common drug-resistant form of this disease. The essential tuberculosis kinase PknB is an attractive drug development target because of its central importance in several critical signaling cascades. A major hurdle in kinase inhibitor development is the reduction of toxicity due to nonspecific kinase activity in host cells. Here a novel class of PknB inhibitors was developed from hit aminopyrimidine 1 (GW779439X), which was originally designed for human CDK4 but failed to progress clinically because of high toxicity and low specificity. Replacing the pyrazolopyridazine headgroup of the original hit with substituted pyridine or phenyl headgroups resulted in a reduction of Cdk activity and a 3-fold improvement in specificity over the human kinome while maintaining PknB activity. This also resulted in improved microbiological activity and reduced toxicity in THP-1 cells and zebrafish. American Chemical Society 2021-01-13 /pmc/articles/PMC8757511/ /pubmed/35035774 http://dx.doi.org/10.1021/acsmedchemlett.0c00580 Text en © 2021 The Authors. Published by American Chemical Society https://pubs.acs.org/page/policy/authorchoice_ccbyncnd_termsofuse.htmlThis is an open access article published under a Creative Commons Non-Commercial No Derivative Works (CC-BY-NC-ND) Attribution License (https://pubs.acs.org/page/policy/authorchoice_ccbyncnd_termsofuse.html) , which permits copying and redistribution of the article, and creation of adaptations, all for non-commercial purposes.
spellingShingle Wlodarchak, Nathan
Feltenberger, John B.
Ye, Zhengqing
Beczkiewicz, Jeffrey
Procknow, Rebecca
Yan, Gang
King, Troy M.
Golden, Jennifer E.
Striker, Rob
Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title_full Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title_fullStr Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title_full_unstemmed Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title_short Engineering Selectivity for Reduced Toxicity of Bacterial Kinase Inhibitors Using Structure-Guided Medicinal Chemistry
title_sort engineering selectivity for reduced toxicity of bacterial kinase inhibitors using structure-guided medicinal chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8757511/
https://www.ncbi.nlm.nih.gov/pubmed/35035774
http://dx.doi.org/10.1021/acsmedchemlett.0c00580
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