1998
DOI: 10.1159/000025310
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Human Immunodeficiency Virus Type 1 Long Terminal Repeat Quasispecies Differ in Basal Transcription and Nuclear Factor Recruitment in Human Glial Cells and Lymphocytes

Abstract: The generation of genomic diversity during the course of infection has the potential to affect all aspects of HIV-1 replication, including expression of the proviral genome. To gain a better understanding of the impact of long terminal repeat (LTR) sequence diversity on LTR-directed gene expression in cells of the central nervous system (CNS) and immune system, we amplified and cloned LTRs from proviral DNA in HIV-1-infected peripheral blood. Sequence analysis of nineteen LTRs cloned from 2 adult and 3 pediatr… Show more

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“…This LEF-1binding site duplication also occurs in ϳ38% of HIV-infected patients within the Vancouver Lymphadenopathy-AIDS Study [182]. Sequence variations in the ATF/CREB-binding site also impact transcription factor recruitment and result in more active isolates [183]. Mutations in the NRRE, which result in the loss of COUP-TF binding in the brain-derived JR-FL strain of the subtype B, do not significantly alter transcription [11].…”
Section: Variability Of the Ltr Modulatory Regionmentioning
confidence: 99%
“…This LEF-1binding site duplication also occurs in ϳ38% of HIV-infected patients within the Vancouver Lymphadenopathy-AIDS Study [182]. Sequence variations in the ATF/CREB-binding site also impact transcription factor recruitment and result in more active isolates [183]. Mutations in the NRRE, which result in the loss of COUP-TF binding in the brain-derived JR-FL strain of the subtype B, do not significantly alter transcription [11].…”
Section: Variability Of the Ltr Modulatory Regionmentioning
confidence: 99%