Yersinia pestis, Yersinia pseudotuberculosis and Yersinia enterocolitica, utilize a plasmid encoded type III secretion system (T3SS) to promote infection by delivering Yersinia outer proteins (Yops) into the cytosol of mammalian cells. This T3SS is absolutely required for Yersinia virulence, which makes T3SS an attractive target in the development of novel therapeutics for treatment of plague and other Yersinia infections. III this Study, a new method for high throughput screening (HTS) of small molecules for the ability to inhibit type I I I secretion (T3S) in Y. pestis has been developed. III comparison with screening assays employed by others, this method is very simple and rapid, and thus well suited for examining very large compound sets. Using this method, we screened a diverse collection of libraries at the US National Screening Laboratory. The initial examination of 70,966 compounds and mixtures from 13 libraries resulted in 43 1 primary hits. Strong positive indications of inhibition were observed at a rate of 0.01%, while moderate and weak but potentially meaningful signals were observed at rates of 0.056% and 0.54% respectively. Further characterizations were conducted on selected primary hits in Y. pestis. Of the eight compounds examined in secondary assays, four show good promise as leads for structure activity relationship studies. They are a diverse group, each having chemical scaffolds not only distinct from one another, but also distinct from previously described candidate T3S inhibitors.
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China Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R ChinaChina Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
Bie, Pengfei
Yang, Xiaowen
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China Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
Chinese Ctr Dis Control & Prevent, State Key Lab Infect Dis Prevent & Control, Collaborat Innovat Ctr Diag & Treatment Infect Di, Natl Inst Communicable Dis Control & Prevent, Beijing, Peoples R ChinaChina Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
Yang, Xiaowen
Zhang, Cunrui
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China Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
China Anim Dis Control Ctr, Beijing, Peoples R ChinaChina Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
Zhang, Cunrui
Wu, Qingmin
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China Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R ChinaChina Agr Univ, Dept Prevent Vet Med, Coll Vet Med, Beijing, Peoples R China
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Univ Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Merck Sharp & Dohme UK Ltd, London, EnglandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Monaghan, Amy E.
Porter, Alison
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Univ Dundee, European Screening Ctr ESC, Dundee, Lanark, Scotland
BioAscent Discovery Ltd, Motherwell, Lanark, ScotlandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Porter, Alison
Hunter, Irene.
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Univ Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, ScotlandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Hunter, Irene.
Morrison, Angus
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Univ Dundee, European Screening Ctr ESC, Dundee, Lanark, Scotland
BioAscent Discovery Ltd, Motherwell, Lanark, ScotlandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Morrison, Angus
McElroy, Stuart P.
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Univ Dundee, European Screening Ctr ESC, Dundee, Lanark, Scotland
BioAscent Discovery Ltd, Motherwell, Lanark, ScotlandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
McElroy, Stuart P.
McEwan, Iain J.
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Univ Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland
Univ Aberdeen, Inst Med Sci, Sch Med, Med Sci & Nutr, Foresterhill, Aberdeen, ScotlandUniv Aberdeen, Inst Med Sci, Sch Med Med Sci & Nutr, Aberdeen, Scotland