Literature DB >> 16571827

Apoptosis of liver-derived cells induced by parvovirus B19 nonstructural protein.

Brian D Poole1, Jing Zhou, Amy Grote, Adam Schiffenbauer, Stanley J Naides.   

Abstract

Parvovirus B19 has been implicated in some cases of acute fulminant non-A, non-B, non-C, non-G liver failure. Our laboratory previously demonstrated that B19 infection of hepatocytes induces apoptosis and that the B19 viral nonstructural protein, NS1, may play a critical role. To study the involvement of NS1 in apoptosis of liver cells, we generated a fusion protein of NS1 with enhanced green fluorescent protein (eGFP) in a system allowing for inducible gene expression. Transfection of the liver-derived cell line HepG2 with the eGFP/NS1 vector allowed expression of the fusion protein, which was visualized by fluorescence microscopy and demonstrated by immunoblotting. The fusion protein localized to discrete domains in the nucleus. Transfection of HepG2 cells with the eGFP/NS1 vector led to apoptosis of 35% of transfected cells, a sevenfold increase over cells transfected with the parent eGFP expression vector. Mutation of the eGFP/NS1 vector to eliminate the nucleoside triphosphate-binding site of NS1 significantly decreased apoptosis, as did treatment of transfected cells with inhibitors of caspase 3 or 9. Neutralization of tumor necrosis factor alpha or Fas ligand had no effect on apoptosis. These results demonstrate that NS1 is sufficient to induce apoptosis in liver-derived cells and that it does so through the initiation of an intrinsic caspase pathway.

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Year:  2006        PMID: 16571827      PMCID: PMC1440431          DOI: 10.1128/JVI.80.8.4114-4121.2006

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  33 in total

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2.  The 3' untranslated region of the B19 parvovirus capsid protein mRNAs inhibits its own mRNA translation in nonpermissive cells.

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4.  Human parvovirus B19 infection in acute fulminant liver failure.

Authors:  Y V Karetnyi; P R Beck; R S Markin; A N Langnas; S J Naides
Journal:  Arch Virol       Date:  1999       Impact factor: 2.574

5.  Hepatitis B virus X protein modulates the apoptosis of hepatoma cell line induced by TRAIL.

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Journal:  Sci China C Life Sci       Date:  2005-06

6.  Possible interactions between the NS-1 protein and tumor necrosis factor alpha pathways in erythroid cell apoptosis induced by human parvovirus B19.

Authors:  N Sol; J Le Junter; I Vassias; J M Freyssinier; A Thomas; A F Prigent; B B Rudkin; S Fichelson; F Morinet
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Authors:  M Muzio; A M Chinnaiyan; F C Kischkel; K O'Rourke; A Shevchenko; J Ni; C Scaffidi; J D Bretz; M Zhang; R Gentz; M Mann; P H Krammer; M E Peter; V M Dixit
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10.  Pro-caspase-3 is a major physiologic target of caspase-8.

Authors:  H R Stennicke; J M Jürgensmeier; H Shin; Q Deveraux; B B Wolf; X Yang; Q Zhou; H M Ellerby; L M Ellerby; D Bredesen; D R Green; J C Reed; C J Froelich; G S Salvesen
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  30 in total

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2.  Viral Nonstructural Protein 1 Induces Mitochondrion-Mediated Apoptosis in Mink Enteritis Virus Infection.

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3.  Epidemiological and clinical characteristics of human parvovirus B19 infections during 2006-2009 in Northern Greece.

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4.  Role of erythropoietin receptor signaling in parvovirus B19 replication in human erythroid progenitor cells.

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5.  miRNA as activity markers in Parvo B19 associated heart disease.

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6.  Parvovirus infection-induced cell death and cell cycle arrest.

Authors:  Aaron Yun Chen; Jianming Qiu
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Review 7.  Human Parvoviruses.

Authors:  Jianming Qiu; Maria Söderlund-Venermo; Neal S Young
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8.  Characterization of erythrovirus B19 genomes isolated in liver tissues from patients with fulminant hepatitis and biliary atresia who underwent liver transplantation.

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9.  Parvovirus B19 genotype specific amino acid substitution in NS1 reduces the protein's cytotoxicity in culture.

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10.  The small 11 kDa nonstructural protein of human parvovirus B19 plays a key role in inducing apoptosis during B19 virus infection of primary erythroid progenitor cells.

Authors:  Aaron Yun Chen; Elizabeth Yan Zhang; Wuxiang Guan; Fang Cheng; Steve Kleiboeker; Thomas M Yankee; Jianming Qiu
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