Literature DB >> 20560978

Derivatives of salicylic acid as inhibitors of YopH in Yersinia pestis.

Zunnan Huang1, Yantao He, Xian Zhang, Andrea Gunawan, Li Wu, Zhong-Yin Zhang, Chung F Wong.   

Abstract

Yersinia pestis causes diseases ranging from gastrointestinal syndromes to bubonic plague and could be misused as a biological weapon. As its protein tyrosine phosphatase YopH has already been demonstrated as a potential drug target, we have developed two series of forty salicylic acid derivatives and found sixteen to have micromolar inhibitory activity. We designed these ligands to have two chemical moieties connected by a flexible hydrocarbon linker to target two pockets in the active site of the protein to achieve binding affinity and selectivity. One moiety possessed the salicylic acid core intending to target the phosphotyrosine-binding pocket. The other moiety contained different chemical fragments meant to target a nearby secondary pocket. The two series of compounds differed by having hydrocarbon linkers with different lengths. Before experimental co-crystal structures are available, we have performed molecular docking to predict how these compounds might bind to the protein and to generate structural models for performing binding affinity calculation to aid future optimization of these series of compounds.

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Year:  2010        PMID: 20560978      PMCID: PMC2908532          DOI: 10.1111/j.1747-0285.2010.00996.x

Source DB:  PubMed          Journal:  Chem Biol Drug Des        ISSN: 1747-0277            Impact factor:   2.817


  33 in total

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4.  A mining minima approach to exploring the docking pathways of p-nitrocatechol sulfate to YopH.

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5.  Conformational selection of protein kinase A revealed by flexible-ligand flexible-protein docking.

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6.  Protein tyrosine phosphatase activity of an essential virulence determinant in Yersinia.

Authors:  K L Guan; J E Dixon
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7.  Multidrug resistance in Yersinia pestis mediated by a transferable plasmid.

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8.  Structure-based discovery of small molecule inhibitors targeted to protein tyrosine phosphatase 1B.

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10.  Aurintricarboxylic acid blocks in vitro and in vivo activity of YopH, an essential virulent factor of Yersinia pestis, the agent of plague.

Authors:  Fubo Liang; Zhonghui Huang; Seung-Yub Lee; Jiao Liang; Maya I Ivanov; Andres Alonso; James B Bliska; David S Lawrence; Tomas Mustelin; Zhong-Yin Zhang
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  11 in total

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6.  EDock-ML: A web server for using ensemble docking with machine learning to aid drug discovery.

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Review 7.  Antibiotic Therapy of Plague: A Review.

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8.  Redox process is crucial for inhibitory properties of aurintricarboxylic acid against activity of YopH: virulence factor of Yersinia pestis.

Authors:  Alicja Kuban-Jankowska; Kamlesh K Sahu; Pawel Niedzialkowski; Magdalena Gorska; Jack A Tuszynski; Tadeusz Ossowski; Michal Wozniak
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9.  Nitropropenyl benzodioxole, an anti-infective agent with action as a protein tyrosine phosphatase inhibitor.

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10.  Aurintricarboxylic acid structure modifications lead to reduction of inhibitory properties against virulence factor YopH and higher cytotoxicity.

Authors:  Alicja Kuban-Jankowska; Kamlesh K Sahu; Magdalena Gorska; Pawel Niedzialkowski; Jack A Tuszynski; Tadeusz Ossowski; Michal Wozniak
Journal:  World J Microbiol Biotechnol       Date:  2016-08-25       Impact factor: 3.312

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