Literature DB >> 9782336

Expression of the fgl2 and its protein product (prothrombinase) in tissues during murine hepatitis virus strain-3 (MHV-3) infection.

J W Ding1, Q Ning, M F Liu, A Lai, K Peltekian, L Fung, C Holloway, H Yeger, M J Phillips, G A Levy.   

Abstract

Murine Hepatitis Virus Strain 3 (MHV-3) produces fulminant hepatitis with 80-90% mortality in Balb/cJ mice. Previous studies in our laboratory have shown that peritoneal macrophages from MHV-3 infected mice produce a procoagulant (PCA) which has the ability to cleave prothrombin to thrombin (prothrombinase) encoded by the gene fgl2 located on chromosome 5. PCA accounts for sinusoidal thrombosis and hepatic necrosis and the necrosis and mortality can be prevented by treatment of animals with a monoclonal antibody to PCA. These present studies were designed to examine the expression of this gene (mRNA by Northern analysis and in situ hybridization) and the gene product PCA (immunochemistry) in tissues recovered from MHV-3 infected Balb/cJ mice in an attempt to explain the liver specific nature of MHV-3 disease. Fgl2 gene expression was detected as early as 8 hours after MHV-3 infection which persisted to 48 hours in the liver, spleen and lungs whereas no gene expression was seen in the brain or kidneys despite the fact that equivalent viral titers were detected in all tissues at all times. In the liver, fgl2 gene expression was confined to endothelial and Kupffer cells with no expression in hepatocytes. Immunochemistry localized the PCA protein to Kupffer cells and endothelial cells and necrotic foci within the liver. No PCA protein was detected by immunochemistry in any other tissues at any time during the course of MHV-3 infection. These results explain the liver specific nature (fulminant hepatitis) of MHV-3 infection and provides further evidence for the role of PCA in the pathogenesis of fulminant hepatitis. MHV-3 induces selective transcription of the gene fgl2 and only hepatic reticuloendothelial cells produce functional protein (PCA) which is known to account for fulminant hepatic failure produced by MHV-3.

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Year:  1998        PMID: 9782336     DOI: 10.1007/978-1-4615-5331-1_79

Source DB:  PubMed          Journal:  Adv Exp Med Biol        ISSN: 0065-2598            Impact factor:   2.622


  15 in total

1.  A disparate subset of double-negative T cells contributes to the outcome of murine fulminant viral hepatitis via effector molecule fibrinogen-like protein 2.

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Journal:  J Virol       Date:  2006-11       Impact factor: 5.103

3.  Physiological functions and clinical implications of fibrinogen-like 2: A review.

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Journal:  World J Clin Infect Dis       Date:  2013-08-25

Review 4.  Coronavirus pathogenesis.

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5.  The murine coronavirus nucleocapsid gene is a determinant of virulence.

Authors:  Timothy J Cowley; Simon Y Long; Susan R Weiss
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6.  Correlation of fibrinogen-like protein 2 with progression of acute pancreatitis in rats.

Authors:  Xiao-Hua Ye; Tan-Zhou Chen; Jia-Ping Huai; Guang-Rong Lu; Xiao-Ju Zhuge; Ren-Pin Chen; Wu-Jie Chen; Chen Wang; Zhi-Ming Huang
Journal:  World J Gastroenterol       Date:  2013-04-28       Impact factor: 5.742

7.  Inhibitory function of Tregs via soluble FGL2 in chronic hepatitis B.

Authors:  Li Xu; Daofeng Yang; Yanlin Liu; Di Wu; Xiaojing Wang; Qin Ning
Journal:  J Huazhong Univ Sci Technolog Med Sci       Date:  2012-08-11

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Authors:  Kai Su; Fang Chen; Wei-Ming Yan; Qi-Li Zeng; Li Xu; Dong Xi; Bin Pi; Xiao-Ping Luo; Qin Ning
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9.  Programmed death (PD)-1-deficient mice are extremely sensitive to murine hepatitis virus strain-3 (MHV-3) infection.

Authors:  Yongwen Chen; Shengxi Wu; Guoning Guo; Lei Fei; Sheng Guo; Chengying Yang; Xiaolan Fu; Yuzhang Wu
Journal:  PLoS Pathog       Date:  2011-07-07       Impact factor: 6.823

10.  Clara Cell 10 kDa Protein Alleviates Murine Hepatitis Virus Strain 3-Induced Fulminant Hepatitis by Inhibiting Fibrinogen-Like Protein 2 Expression.

Authors:  Haijing Yu; Yang Liu; Hongwu Wang; Xiaoyang Wan; Jiaquan Huang; Weiming Yan; Dong Xi; Xiaoping Luo; Guanxin Shen; Qin Ning
Journal:  Front Immunol       Date:  2018-12-13       Impact factor: 7.561

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