Your search keyword '"Fenyong Liu"' showing total 206 results

201. Two Gamma Interferon-Activated Site-Like Elements in the Human Cytomegalovirus Major Immediate-Early Promoter/Enhancer Are Important for Viral Replication.

Author

Netterwald, James, Shaojun Yang, Weijia Wang, Ghanny, Salena, Cody, Michael, Soteropoulos, Patricia, Bin Tian, Dunn, Walter, Fenyong Liu, and Hua Zhu

Subjects

*CYTOMEGALOVIRUSES, *VIRAL replication, *INTERFERONS, *PROMOTERS (Genetics), *GENE expression, *VIRAL genomes

Abstract

Human cytomegalovirus (HCMV) infection directly initiates a signal transduction pathway that leads to activation of a large number of cellular interferon-stimulated genes (ISGs). Our previous studies demonstrated that two interferon response elements, the interferon-stimulated response element and gamma interferon-activated site (GAS), in the ISG promoters serve as HCMV response sites (VRS). Interestingly, two GAS-like VRS elements (VRS1) were also present in the HCMV major immediate-early promoter-enhancer (MIEP/E). In this study, the importance of these VRS elements in viral replication was investigated. We demonstrate that the expression of the major IE genes, IE1 and IE2, is interferon inducible. To understand the biological significance of this signal transduction pathway in HCMV major IE expression, the two VRS1 in the MIEP/E were mutated. Mutant HCMVs in which the VRS elements were deleted or that contained point mutations grew dramatically more slowly than wild-type virus at a low multiplicity of infection (MOI). Insertion of wild-type VRS1 into the mutant viral genome rescued the slow growth phenotype. Furthermore, the expression levels of major IE RNAs and proteins were greatly reduced during infection with the VRS mutants at a low MOI. HCMV microarray analysis indicated that infection of host cells with the VRS mutant virus resulted in a global reduction in the expression of viral genes. Collectively, these data demonstrate that the two VRS elements in the MIEP/E are necessary for efficient viral gene expression and replication. This study suggests that although the HCMV-initiated signal transduction pathway results in induction of cellular antiviral genes, it also functions to stimulate viral major IE gene expression. This might be a new viral strategy in which the pathway is used to regulate gene expression and play a role in reactivation. [ABSTRACT FROM AUTHOR]

Published

2005

202. Murine Cytomegalovirus with a Transposon Insertional Mutation at Open Reading Frame m155 Is Deficient in Growth and Virulence in Mice.

Author

Abenes, Gerardo, Chan, Karen, Lee, Manfred, Haghjoo, Erik, Jiaming Zhu, Tianhong Zhou, Xiaoyan Zhan, and Fenyong Liu

Subjects

*CYTOMEGALOVIRUSES, *TRANSPOSONS, *LABORATORY mice, *GENETIC mutation, *VIRAL replication, *COMMUNICABLE diseases, *VIROLOGY

Abstract

A pool of murine cytomegalovirus (MCMV) mutants was previously generated by using a Tn3-based transposon mutagenesis approach (X. Zhan, M. Lee, J. Xiao, and F. Liu, J. Virol. 74:7411–7421, 2000). In this study, one of the MCMV mutants, Rvm155, which contained the transposon insertion in open reading frame m155, was characterized in vitro for its replication in tissue culture and in vivo for its growth and virulence in immunodeficient SCID mice. Compared to the wild-type strain and a rescued virus that restored the m155 region, the mutant is significantly deficient in growth in many organs of the infected animals. At 21 days postinfection the titers of Rvm155 in the salivary glands, lungs, spleens, livers, and kidneys of the intraperitoneally infected SCID mice were lower than the titers of the wild-type virus and the rescued virus by 50-, 1,000-, 500-, 100-, and 500-fold, respectively. Moreover, the viral mutant was attenuated in killing the SCID mice, as none of the SCID mice that were intraperitoneally infected with Rvm155 died until 38 days postinfection while all the animals infected with the wild-type and rescued viruses died at 27 days postinfection. Our results provide the first direct evidence that a disruption of m155 expression leads to attenuation of viral virulence and growth in animals. Moreover, these results suggest that m155 is a viral determinant for optimal MCMV growth and virulence in vivo. [ABSTRACT FROM AUTHOR]

Published

2004

203. Engineered RNase P Ribozymes Are Efficient in Cleaving a Human Cytomegalovirus mRNA in Vitro and Are Effective in Inhibiting Viral Gene Expression and Growth in Human Cells.

Author

Hua Zou, Lee, Jarone, Umamoto, Sean, Kilani, Ahmed F., Kim, Joseph, Phong Trang, Tianhong Zhou, and Fenyong Liu

Subjects

*CATALYTIC RNA, *MESSENGER RNA, *CYTOMEGALOVIRUSES, *BIOCHEMISTRY

Abstract

Presents a study where a ribozyme variant was used to target the overlapping region of the mRNA encoding human cytomegalovirus major transcription regulatory proteins IE1 and IE2. Efficiency of the variant in cleaving the IE1/IE2 mRNA sequence in vitro over the ribozyme derived from the wild type RNase P ribozyme; Reduction in viral growth in cells that either did not express the ribozyme or produced a catalytically inactive ribozyme mutant.

Published

2003

204. Murine Cytomegalovirus with a Transposon Insertional Mutation at Open Reading Frame M35 Is Defective in Growth In Vivo.

Author

Tam, Ada, Jiaming Zhu, Rong Hai, Haghjoo, Erik, Tuong Tong, Xiaoyan Zhan, Sangwei Lu, and Fenyong Liu

Subjects

*CYTOMEGALOVIRUS diseases, *GENETIC mutation, *TRANSPOSONS, *TISSUE culture, *LABORATORY mice

Abstract

We had previously constructed a pool of murine cytomegalovirus (MCMV) mutants that contained a Tn3-based transposon sequence randomly inserted in the viral genome. In the study reported here, one of the mutants, RvM35, which contains the transposon insertion at open reading frame M35, was characterized both in vitro in tissue cultures and in immunocompetent Balb/c and immunodeficient SCID mice. Our results provide the first direct evidence to suggest that M35 is not essential for viral replication in vitro in NIH 3T3 cells. Compared to the wild-type strain and a rescued virus that restored the M35 region, the viral mutant was attenuated in growth in both the intraperitoneally infected Balb/c and SCID mice. At 21 days postinfection, the titers of the mutant in the salivary glands, lungs, spleens, livers, and kidneys of the SCID mice were lower than the titers of the wild-type Smith strain and the rescued virus by 50,000-, 100-, 10-, 100-, and 50-fold, respectively. Moreover, the growth of RvM35 is severely attenuated in the salivary glands. The virulence of the mutant virus also appears to be attenuated, because no death was observed in SCID mice infected with RvM35 until 35 days postinfection, while all the animals infected with the wild-type and rescued viruses died 27 days postinfection. Our results suggest that M35 is important for MCMV virulence in killing SCID mice and is required for optimal viral growth in vivo, including in the salivary glands. [ABSTRACT FROM AUTHOR]

Published

2003

205. In Vitro and In Vivo Characterization of a Murine Cytomegalovirus with a Mutation at Open Reading Frame m166.

Author

Jiaming Zhu, Chen, Jennifer, Rong Hai, Tuong Tong, Jianqiao Xiao, Xiaoyan Zhan, Sangwei Lu, and Fenyong Liu

Subjects

*CYTOMEGALOVIRUSES, *TRANSPOSONS, *MUTAGENESIS

Abstract

We have recently generated a pool of murine cytomegalovirus (MCMV) mutants by using a Tn3-based transposon mutagenesis approach. In this study, one of the mutants, Rvm166, which contained the transposon sequence at open reading frame m166, was characterized both in tissue culture and in immunocompetent BALB/c mice and immunodeficient SCID mice. The viral mutant replicated as well as the wild-type Smith strain in vitro in NIH 3T3 cells, whereas the transposon insertion precluded the expression of >65% of the m166 open reading frame. Compared to the wild-type strain and a rescued virus that restored the m166 region, the viral mutant was significantly attenuated in growth in both BALB/c and SCID mice that were intraperitoneally infected with the viruses. At 21 days postinfection, the titers of the viral mutant in the salivary glands, lungs, spleens, livers, and kidneys of the infected SCID mice were lower than the titers of the Smith strain and the rescued virus by about 30,000-, 10,000-, 1,000-, 300-, and 800-fold, respectively. Moreover, the virulence of the mutant virus appears to be severely attenuated because no death was found in SCID mice infected with the viral mutant up to 90 days postinfection, whereas all of the animals infected with the wild-type and rescued viruses died at 27 days postinfection. Our results suggest that m166 probably encodes a virulence factor and is required for MCMV virulence in killing SCID mice and for optimal viral growth in vivo. [ABSTRACT FROM AUTHOR]

Published

2003

206. Human Cytomegalovirus Primase UL70 Specifically Interacts with Cellular Factor Snapin.

Author

Ao Shen, Ji Lei, Yang, Edward, Yonggang Pei, Yuan-Chuan Chen, Hao Gong, Gengfu Xiao, and Fenyong Liu

Subjects

*CYTOMEGALOVIRUS diseases, *GENES, *DNA synthesis, *MOLECULES, *RNA

Abstract

Genomic DNA synthesis is a universally conserved process for all herpesviruses, including human cytomegalovirus (HCMV). HCMV UL70 is believed to encode the primase of the DNA replication machinery, a function which requires localization in the nucleus, the site of viral DNA synthesis. No host factors that interact with UL70 have been reported. In this study, we provide the first direct evidence that UL70 specifically interacts with Snapin, a human protein that is predominantly localized in the cytoplasm and is associated with cellular vesicles. The interaction between UL70 and Snapin was identified in both the two-hybrid screen in yeast and coimmunoprecipitation in human cells. The nuclear import of UL70 was decreased in cells overexpressing Snapin and increased in cells in which the expression of Snapin was downregulated with anti-Snapin small interfering RNA (siRNA) molecules, respectively. Furthermore, viral DNA synthesis and progeny production were decreased in cells overexpressing Snapin and increased in the anti- Snapin siRNA-treated cells, respectively. In contrast, no significant difference in the nuclear level of UL70, viral DNA synthesis, and progeny production was found among the parental cells and cells that either expressed a control empty vector or were treated with control siRNA molecules that did not recognize any viral or cellular transcripts. Our results suggest that Snapin may play a key role in regulating the cellular localization of UL70 in HCMV, leading to modulation of viral DNA synthesis and progeny production. [ABSTRACT FROM AUTHOR]

Published

2011