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Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection

[Image: see text] Every year three million people die as a result of bacterial infections, and this number may further increase due to resistance to current antibiotics. These antibiotics target almost all essential bacterial processes, leaving only a few new targets for manipulation. The host prote...

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Autores principales: Albers, Harald M. H. G., Kuijl, Coenraad, Bakker, Jeroen, Hendrickx, Loes, Wekker, Sharida, Farhou, Nadha, Liu, Nora, Blasco-Moreno, Bernat, Scanu, Tiziana, den Hertog, Jeroen, Celie, Patrick, Ovaa, Huib, Neefjes, Jacques
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2013
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3934374/
https://www.ncbi.nlm.nih.gov/pubmed/24274083
http://dx.doi.org/10.1021/cb400421a
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author Albers, Harald M. H. G.
Kuijl, Coenraad
Bakker, Jeroen
Hendrickx, Loes
Wekker, Sharida
Farhou, Nadha
Liu, Nora
Blasco-Moreno, Bernat
Scanu, Tiziana
den Hertog, Jeroen
Celie, Patrick
Ovaa, Huib
Neefjes, Jacques
author_facet Albers, Harald M. H. G.
Kuijl, Coenraad
Bakker, Jeroen
Hendrickx, Loes
Wekker, Sharida
Farhou, Nadha
Liu, Nora
Blasco-Moreno, Bernat
Scanu, Tiziana
den Hertog, Jeroen
Celie, Patrick
Ovaa, Huib
Neefjes, Jacques
author_sort Albers, Harald M. H. G.
collection PubMed
description [Image: see text] Every year three million people die as a result of bacterial infections, and this number may further increase due to resistance to current antibiotics. These antibiotics target almost all essential bacterial processes, leaving only a few new targets for manipulation. The host proteome has many more potential targets for manipulation in order to control bacterial infection, as exemplified by the observation that inhibiting the host kinase Akt supports the elimination of different intracellular bacteria including Salmonella and M. tuberculosis. If host kinases are involved in the control of bacterial infections, phosphatases could be as well. Here we present an integrated small interference RNA and small molecule screen to identify host phosphatase-inhibitor combinations that control bacterial infection. We define host phosphatases inhibiting intracellular growth of Salmonella and identify corresponding inhibitors for the dual specificity phosphatases DUSP11 and 27. Pathway analysis places many kinases and phosphatases controlling bacterial infection in an integrated pathway centered around Akt. This network controls host cell metabolism, survival, and growth and bacterial survival and reflect a natural host cell response to bacterial infection. Inhibiting two enzyme classes with opposite activities–kinases and phosphatases–may be a new strategy to overcome infections by antibiotic-resistant bacteria.
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spelling pubmed-39343742014-02-25 Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection Albers, Harald M. H. G. Kuijl, Coenraad Bakker, Jeroen Hendrickx, Loes Wekker, Sharida Farhou, Nadha Liu, Nora Blasco-Moreno, Bernat Scanu, Tiziana den Hertog, Jeroen Celie, Patrick Ovaa, Huib Neefjes, Jacques ACS Chem Biol [Image: see text] Every year three million people die as a result of bacterial infections, and this number may further increase due to resistance to current antibiotics. These antibiotics target almost all essential bacterial processes, leaving only a few new targets for manipulation. The host proteome has many more potential targets for manipulation in order to control bacterial infection, as exemplified by the observation that inhibiting the host kinase Akt supports the elimination of different intracellular bacteria including Salmonella and M. tuberculosis. If host kinases are involved in the control of bacterial infections, phosphatases could be as well. Here we present an integrated small interference RNA and small molecule screen to identify host phosphatase-inhibitor combinations that control bacterial infection. We define host phosphatases inhibiting intracellular growth of Salmonella and identify corresponding inhibitors for the dual specificity phosphatases DUSP11 and 27. Pathway analysis places many kinases and phosphatases controlling bacterial infection in an integrated pathway centered around Akt. This network controls host cell metabolism, survival, and growth and bacterial survival and reflect a natural host cell response to bacterial infection. Inhibiting two enzyme classes with opposite activities–kinases and phosphatases–may be a new strategy to overcome infections by antibiotic-resistant bacteria. American Chemical Society 2013-11-25 2014-02-21 /pmc/articles/PMC3934374/ /pubmed/24274083 http://dx.doi.org/10.1021/cb400421a Text en Copyright © 2013 American Chemical Society Terms of Use (http://pubs.acs.org/page/policy/authorchoice_termsofuse.html)
spellingShingle Albers, Harald M. H. G.
Kuijl, Coenraad
Bakker, Jeroen
Hendrickx, Loes
Wekker, Sharida
Farhou, Nadha
Liu, Nora
Blasco-Moreno, Bernat
Scanu, Tiziana
den Hertog, Jeroen
Celie, Patrick
Ovaa, Huib
Neefjes, Jacques
Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title_full Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title_fullStr Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title_full_unstemmed Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title_short Integrating Chemical and Genetic Silencing Strategies To Identify Host Kinase-Phosphatase Inhibitor Networks That Control Bacterial Infection
title_sort integrating chemical and genetic silencing strategies to identify host kinase-phosphatase inhibitor networks that control bacterial infection
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3934374/
https://www.ncbi.nlm.nih.gov/pubmed/24274083
http://dx.doi.org/10.1021/cb400421a
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