Literature DB >> 10559318

Human cytomegalovirus UL144 open reading frame: sequence hypervariability in low-passage clinical isolates.

N S Lurain1, K S Kapell, D D Huang, J A Short, J Paintsil, E Winkfield, C A Benedict, C F Ware, J W Bremer.   

Abstract

Human cytomegalovirus (HCMV) infects a number of organs and cell types in vivo, leading to the hypothesis that HCMV disease and tissue tropism may be related to specific sequence variants. A potential component of HCMV variant strains is the UL144 open reading frame (ORF), which encodes a homologue of the herpesvirus entry mediator, HveA, a member of the tumor necrosis factor receptor superfamily. Sequence analysis of the UL144 ORF in 45 low-passage clinical isolates demonstrated significant strain-specific variability. In individual isolates, nucleotide substitutions occur at up to 21% of the 531 positions, resulting in approximately the same percentage of substitutions in the predicted 176-amino-acid sequence. Phylogenetic analysis indicated that the nucleotide and amino acid sequences diverge into three major groups. For genotypic comparison, the known hypervariable region encompassing the proteolytic cleavage site of the glycoprotein B (gB) gene was also sequenced. All of the isolates could be typed according to the four known gB groups; however, the gB and UL144 sequence groups appeared to be phylogenetically unlinked. The predicted UL144 product homology with tumor necrosis factor receptor family members, along with the unexpectedly high level of sequence variability of the UL144 ORF, suggests that the predicted product may play a role in HCMV infectivity and subsequent host disease.

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Year:  1999        PMID: 10559318      PMCID: PMC113055     

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


  54 in total

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  45 in total

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7.  Human cytomegalovirus and human immunodeficiency virus type-1 co-infection in human cervical tissue.

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8.  HIV type 1 and cytomegalovirus coinfection in the female genital tract.

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