2006
DOI: 10.1002/jgm.908
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Gene therapy for HIV infection: what does it need to make it work?

Abstract: The efficacy of antiviral drug therapy for HIV infection is limited by toxicity and viral resistance. Thus, alternative therapies need to be explored. Several gene therapeutic strategies for HIV infection have been developed, but in clinical testing therapeutically effective levels of the transgene product were not achieved. This review focuses on the determinants of therapeutic efficacy and discusses the potential and also the limits of current gene therapy approaches for HIV infection.

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Cited by 47 publications
(32 citation statements)
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“…As an RNA virus, HIV is a target of choice because Rzs may target both the incoming RNA in newly infected cells and the RNA produced during the replicating cycle. 15,47 The design of SOFA-HDV Rzs should correspond to criteria of new compounds with improved efficacy and stability. The in vitro activity of the computer-designed SOFA-HDV-Rzs shows that new active compounds have been obtained (Figs.…”
Section: Methodsmentioning
confidence: 99%
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“…As an RNA virus, HIV is a target of choice because Rzs may target both the incoming RNA in newly infected cells and the RNA produced during the replicating cycle. 15,47 The design of SOFA-HDV Rzs should correspond to criteria of new compounds with improved efficacy and stability. The in vitro activity of the computer-designed SOFA-HDV-Rzs shows that new active compounds have been obtained (Figs.…”
Section: Methodsmentioning
confidence: 99%
“…12 Hammerhead and hairpin Rzs are currently in clinical trials against HIV, expressed from murine retroviral or lentiviral vectors. [13][14][15] Therefore, Rzs appear to have a great potential for further development of a gene-inactivation system aiming to control HIV propagation.…”
Section: In Vitro and In Vivo Cleavage Of Hiv-1 Rna By New Sofa-hdv Rmentioning
confidence: 99%
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“…Such approaches target critical steps in the virus life cycle, from blocking virus entry into cells to interfering with the regulation of viral gene expression, as well as priming the immune system. [1][2][3] Introducing genes that limit early steps in viral replication, like virus entry into CD4+ T cells, has the potential to select and expand HIV target cells that are resistant to infection. 2,4 Peptide-based fusion inhibitors derived from HIV gp41 C-terminal hydrophobic a-helix inhibit virus fusion by interacting with the N-terminal hydrophobic a-helix.…”
Section: Introductionmentioning
confidence: 99%
“…[1][2][3] Introducing genes that limit early steps in viral replication, like virus entry into CD4+ T cells, has the potential to select and expand HIV target cells that are resistant to infection. 2,4 Peptide-based fusion inhibitors derived from HIV gp41 C-terminal hydrophobic a-helix inhibit virus fusion by interacting with the N-terminal hydrophobic a-helix. Thus, they block conformational changes essential for membrane fusion of the virus with the host cell.…”
Section: Introductionmentioning
confidence: 99%