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Dusp3 and Psme3 Are Associated with Murine Susceptibility to Staphylococcus aureus Infection and Human Sepsis
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نویسنده
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yan q. ,sharma-kuinkel b.k. ,deshmukh h. ,tsalik e.l. ,cyr d.d. ,lucas j. ,woods c.w. ,scott w.k. ,sempowski g.d. ,thaden j. ,rude t.h. ,ahn s.h. ,fowler jr. v.g.
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منبع
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plos pathogens - 2014 - دوره : 10 - شماره : 6
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چکیده
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Using a/j mice,which are susceptible to staphylococcus aureus,we sought to identify genetic determinants of susceptibility to s. aureus,and evaluate their function with regard to s. aureus infection. one qtl region on chromosome 11 containing 422 genes was found to be significantly associated with susceptibility to s. aureus infection. of these 422 genes,whole genome transcription profiling identified five genes (dcaf7,dusp3,fam134c,psme3,and slc4a1) that were significantly differentially expressed in a) s. aureus -infected susceptible (a/j) vs. resistant (c57bl/6j) mice and b) humans with s. aureus blood stream infection vs. healthy subjects. three of these genes (dcaf7,dusp3,and psme3) were down-regulated in susceptible vs. resistant mice at both pre- and post-infection time points by qpcr. sirna-mediated knockdown of dusp3 and psme3 induced significant increases of cytokine production in s. aureus-challenged raw264.7 macrophages and bone marrow derived macrophages (bmdms) through enhancing nf-κb signaling activity. similar increases in cytokine production and nf-κb activity were also seen in bmdms from css11 (c57bl/6j background with chromosome 11 from a/j),but not c57bl/6j. these findings suggest that dusp3 and psme3 contribute to s. aureus infection susceptibility in a/j mice and play a role in human s. aureus infection.
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آدرس
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division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc, United States, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc, United States, division of neonatology,department of pediatrics,perelman school of medicine,university of pennsylvania,philadelphia,pa, United States, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc,united states,emergency medicine service,durham veteran's affairs medical center,durham,nc,united states,duke institute for genome sciences and policy,duke university,durham,nc, United States, duke institute for genome sciences and policy,duke university,durham,nc, United States, quintiles innovations,morrisville,nc, United States, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc,united states,duke institute for genome sciences and policy,duke university,durham,nc,united states,section on infectious diseases,durham veteran's affairs medical center,durham,nc, United States, hussman institute for human genomics,university of miami miller school of medicine,miami,fl,united states,dr. john t. macdonald foundation department of human genetics,university of miami miller school of medicine,miami,fl, United States, duke human vaccine institute,durham,nc, United States, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc,united states,duke institute for genome sciences and policy,duke university,durham,nc,united states,duke clinical research institute,durham,nc, United States, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc, United States, department of biochemistry school of dentistry,chonnam national university,bukgu,gwangju, South Korea, division of infectious diseases and international health,department of medicine,duke university school of medicine,durham,nc,united states,duke institute for genome sciences and policy,duke university,durham,nc,united states,duke clinical research institute,durham,nc, United States
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Authors
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