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The human polyomavirus BK T antigen induces gene expression in human cytomegalovirus
Co-infections or co-habitations of cells by two or more viruses may occur in the human organism. Human cytomegalovirus (HCMV) and the human polyomavirus BK (BKV) have common host cells and may both establish lifelong latency/persistence following primary infection. Both viruses may become reactivate...
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Published in: | Virus research 1997-11, Vol.52 (1), p.61-71 |
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container_title | Virus research |
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creator | Kristoffersen, Anne K Johnsen, John Inge Seternes, Ole Morten Rollag, Halvor Degré, Miklos Traavik, Terje |
description | Co-infections or co-habitations of cells by two or more viruses may occur in the human organism. Human cytomegalovirus (HCMV) and the human polyomavirus BK (BKV) have common host cells and may both establish lifelong latency/persistence following primary infection. Both viruses may become reactivated by immunosuppression or other conditions which upset host–virus balance, and they encode gene products with the inherent potential of acting as heterologous transacting factors for expression of cellular or viral genes. It has been shown that HCMV induces gene expression and replication of primate polyomaviruses. We now demonstrate that BKV is able to enhance the expression of HCMV immediate early (IE1 and 2) as well as the early (E) protein pp65 during double infections in semi-permissive cells. By transfection experiments it was established that the phenomenon is due to heterologous transcriptional transactivation of the HCMV major IE promoter (MIEP) by the BKV large T antigen, without contribution from the small t antigen. |
doi_str_mv | 10.1016/S0168-1702(97)00100-7 |
format | article |
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Human cytomegalovirus (HCMV) and the human polyomavirus BK (BKV) have common host cells and may both establish lifelong latency/persistence following primary infection. Both viruses may become reactivated by immunosuppression or other conditions which upset host–virus balance, and they encode gene products with the inherent potential of acting as heterologous transacting factors for expression of cellular or viral genes. It has been shown that HCMV induces gene expression and replication of primate polyomaviruses. We now demonstrate that BKV is able to enhance the expression of HCMV immediate early (IE1 and 2) as well as the early (E) protein pp65 during double infections in semi-permissive cells. 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Human cytomegalovirus (HCMV) and the human polyomavirus BK (BKV) have common host cells and may both establish lifelong latency/persistence following primary infection. Both viruses may become reactivated by immunosuppression or other conditions which upset host–virus balance, and they encode gene products with the inherent potential of acting as heterologous transacting factors for expression of cellular or viral genes. It has been shown that HCMV induces gene expression and replication of primate polyomaviruses. We now demonstrate that BKV is able to enhance the expression of HCMV immediate early (IE1 and 2) as well as the early (E) protein pp65 during double infections in semi-permissive cells. 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subjects | Antigens, Viral, Tumor - physiology BK Virus - immunology BKV BKV large T antigen Cells, Cultured Co-infection Cytomegalovirus - genetics Cytomegalovirus Infections - genetics Cytomegalovirus Infections - virology Enhancer Elements, Genetic Gene Expression Regulation, Viral Genes, Immediate-Early HCMV Humans Promoter Regions, Genetic Transcriptional Activation Transfection Tumor Cells, Cultured |
title | The human polyomavirus BK T antigen induces gene expression in human cytomegalovirus |
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