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   The NLRP3 Inflammasome and IL-1β Accelerate Immunologically Mediated Pathology in Experimental Viral Fulminant Hepatitis  
   
نویسنده guo s. ,yang c. ,diao b. ,huang x. ,jin m. ,chen l. ,yan w. ,ning q. ,zheng l. ,wu y. ,chen y.
منبع plos pathogens - 2015 - دوره : 11 - شماره : 9 - صفحه:1 -21
چکیده    Viral fulminant hepatitis (fh) is a severe disease with high mortality resulting from excessive inflammation in the infected liver. clinical interventions have been inefficient due to the lack of knowledge for inflammatory pathogenesis in the virus-infected liver. we show that wild-type mice infected with murine hepatitis virus strain-3 (mhv-3),a model for viral fh,manifest with severe disease and high mortality in association with a significant elevation in il-1β expression in the serum and liver. whereas,the viral infection in il-1β receptor-i deficient (il-1r1-/-) or il-1r antagonist (il-1ra) treated mice,show reductions in virus replication,disease progress and mortality. il-1r1 deficiency appears to debilitate the virus-induced fibrinogen-like protein-2 (fgl2) production in macrophages and cd45+gr-1high neutrophil infiltration in the liver. the quick release of reactive oxygen species (ros) by the infected macrophages suggests a plausible viral initiation of nlrp3 inflammasome activation. further experiments show that mice deficient of p47phox,a nicotinamide adenine dinucleotide phosphate (nadph) oxidase subunit that controls acute ros production,present with reductions in nlrp3 inflammasome activation and subsequent il-1β secretion during viral infection,which appears to be responsible for acquiring resilience to viral fh. moreover,viral infected animals in deficiencies of nlrp3 and caspase-1,two essential components of the inflammasome complex,also have reduced il-1β induction along with ameliorated hepatitis. our results demonstrate that the ros/nlrp3/il-1β axis institutes an essential signaling pathway,which is over activated and directly causes the severe liver disease during viral infection,which sheds light on development of efficient treatments for human viral fh and other severe inflammatory diseases.
آدرس institute of immunology,pla,third military medical university,chongqing, China, institute of immunology,pla,third military medical university,chongqing, China, institute of immunology,pla,third military medical university,chongqing, China, institute of immunology,pla,third military medical university,chongqing, China, department of pharmacology,yanbian university,yanji,jilin province, China, department of basic medicine,yanbian university,yanji,jilin province, China, department and institute of infectious disease,tongji hospital,tongji medical college,huazhong university of science and technology,wuhan, China, department and institute of infectious disease,tongji hospital,tongji medical college,huazhong university of science and technology,wuhan, China, laboratory of immunology,national institute of allergy and infectious diseases,national institutes of health,bethesda,md, United States, institute of immunology,pla,third military medical university,chongqing, China, institute of immunology,pla,third military medical university,chongqing, China
 
     
   
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