The latent nuclear antigen of Kaposi sarcoma-associated herpesvirus targets the retinoblastoma–E2F pathway and with the oncogene Hras transforms primary rat …

SA Radkov, P Kellam, C Boshoff - Nature medicine, 2000 - nature.com
SA Radkov, P Kellam, C Boshoff
Nature medicine, 2000nature.com
Kaposi sarcoma-associated herpesvirus (KSHV) is involved in the etiopathogenesis of
Kaposi sarcoma and certain lymphoproliferative disorders. Open reading frame (ORF) 73
encodes the main immunogenic latent nuclear antigen (LNA-1) of KSHV. LNA-1 maintains
the KSHV episome and tethers the viral genome to chromatin during mitosis. In addition,
LNA-1 interacts with p53 and represses its transcriptional activity. Here we show that LNA-1
also interacts with the retinoblastoma protein. LNA-1 transactivated an artificial promoter …
Kaposi sarcoma-associated herpesvirus (KSHV) is involved in the etiopathogenesis of Kaposi sarcoma and certain lymphoproliferative disorders. Open reading frame (ORF) 73 encodes the main immunogenic latent nuclear antigen (LNA-1) of KSHV. LNA-1 maintains the KSHV episome and tethers the viral genome to chromatin during mitosis. In addition, LNA-1 interacts with p53 and represses its transcriptional activity. Here we show that LNA-1 also interacts with the retinoblastoma protein. LNA-1 transactivated an artificial promoter carrying the cell cycle transcription factor E2F DNA-binding sequences and also upregulated the cyclin E (CCNE1) promoter, but not the B-myb (MYBL2) promoter. LNA-1 overcame the flat-cell phenotype induced by retinoblastoma protein in Saos2 cells. In cooperation with the cellular oncogene Harvey rat sarcoma viral oncogene homolog (Hras), LNA-1 transformed primary rat embryo fibroblasts and rendered them tumorigenic. These findings indicate that LNA-1 acts as a transcription co-factor and may contribute to KSHV-induced oncogenesis by targeting the retinoblastoma protein–E2F transcriptional regulatory pathway.
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