Literature DB >> 10079251

Murine cytomegalovirus immediate-early promoter directs astrocyte-specific expression in transgenic mice.

S Aiba-Masago1, S Baba, R Y Li, Y Shinmura, I Kosugi, Y Arai, M Nishimura, Y Tsutsui.   

Abstract

Murine cytomegalovirus (MCMV), which causes acute, latent, and persistent infection of the natural host, is used as an animal model of human cytomegalovirus (HCMV) infection. Transcription of MCMV immediate-early (IE) genes is required for expression of the early and late genes and is dependent on host cell transcription factors. Cell-type-specific expression activity of the MCMV IE promoter was analyzed in transgenic mice generated with the major IE (MIE) enhancer/promoter involving nucleotides -1343 to -6 (1338 bp) connected to the reporter gene lacZ. Distinct expression was observed in the brain, kidneys, stomach, and skeletal muscles. Weak expression was observed in a portion of the parenchymal cells of the salivary glands and pancreas, and expression was hardly detected in the lungs, intestine, or immune and hematopoietic organs such as the thymus, spleen, lymph nodes, and bone marrow. The spectrum of organs positive for expression was narrower than that of the HCMV MIE promoter-lacZ transgenic mice reported previously and showed a greater degree of cell-type specificity. Interestingly, astrocyte-specific expression of the transgene was observed in the brain and primary glial cultures from the transgenic mice by combination of beta-galactosidase (beta-Gal) expression and immunostaining for cell markers. However, the transgene was not expressed in neurons, oligodendroglia, microglia, or endothelial cells. Furthermore, the beta-Gal expression in glial cultures was stimulated significantly by MCMV infection or by addition of calcium ionophore. These observations indicated that expression activity of the MCMV IE promoter is strictly cell-type specific, especially astrocyte-specific in the brain. This specific pattern of activity is similar to that of natural HCMV infection in humans.

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Year:  1999        PMID: 10079251      PMCID: PMC1866421          DOI: 10.1016/S0002-9440(10)65320-5

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  43 in total

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3.  The transgenic ICP4 promoter is activated in Schwann cells in trigeminal ganglia of mice latently infected with herpes simplex virus type 1.

Authors:  N S Taus; W J Mitchell
Journal:  J Virol       Date:  2001-11       Impact factor: 5.103

4.  Neurons differentially activate the herpes simplex virus type 1 immediate-early gene ICP0 and ICP27 promoters in transgenic mice.

Authors:  Christie M Loiacono; Robert Myers; William J Mitchell
Journal:  J Virol       Date:  2002-03       Impact factor: 5.103

5.  The herpes simplex virus type 1 early gene (thymidine kinase) promoter is activated in neurons of brain, but not trigeminal ganglia, of transgenic mice in the absence of viral proteins.

Authors:  Christie M Loiacono; Robert Myers; William J Mitchell
Journal:  J Neurovirol       Date:  2004-04       Impact factor: 2.643

6.  Neuron-specific activation of murine cytomegalovirus early gene e1 promoter in transgenic mice.

Authors:  Yoshifumi Arai; Mizuho Ishiwata; Satoshi Baba; Hideya Kawasaki; Isao Kosugi; Ren-Yong Li; Takashi Tsuchida; Katsutoshi Miura; Yoshihiro Tsutsui
Journal:  Am J Pathol       Date:  2003-08       Impact factor: 4.307

7.  Regulation of pulmonary and systemic bacterial lipopolysaccharide responses in transgenic mice expressing human elafin.

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Journal:  Infect Immun       Date:  2003-07       Impact factor: 3.441

8.  Innate immune responses to cytomegalovirus infection in the developing mouse brain and their evasion by virus-infected neurons.

Authors:  Isao Kosugi; Hideya Kawasaki; Yoshifumi Arai; Yoshihiro Tsutsui
Journal:  Am J Pathol       Date:  2002-09       Impact factor: 4.307

9.  Tumorigenic potential of pituitary tumor transforming gene (PTTG) in vivo investigated using a transgenic mouse model, and effects of cross breeding with p53 (+/-) transgenic mice.

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10.  Mouse embryonic stem cells inhibit murine cytomegalovirus infection through a multi-step process.

Authors:  Hideya Kawasaki; Isao Kosugi; Yoshifumi Arai; Toshihide Iwashita; Yoshihiro Tsutsui
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