Literature DB >> 15831707

Lentiviral delivery of short hairpin RNAs protects CD4 T cells from multiple clades and primary isolates of HIV.

Sang-Kyung Lee1, Derek M Dykxhoorn, Priti Kumar, Shahin Ranjbar, Erwei Song, Laura E Maliszewski, Vanessa François-Bongarçon, Anne Goldfeld, N Manjunath Swamy, Judy Lieberman, Premlata Shankar.   

Abstract

Viral heterogeneity is a major hurdle for potential therapeutic use of RNA interference (RNAi) against HIV-1. To determine the extent of RNAi tolerance to mutations, we tested 3 viral target sites with differing propensity for mutations: a highly variable rev sequence, a gag sequence conserved only among clade B isolates, and a vif sequence highly conserved across clades. Lentiviral expression of all 3 shRNAs inhibited replication of the homologous HIV(IIIB) strain. However, they differed in their ability to protect primary CD4 T cells against multiple isolates within and across HIV clades. The least conserved rev sequence inhibited only 2 of 5 clade B isolates. The gag sequence (conserved within clade B) protected 5 of 5 clade B isolates but not other clade viruses with 2 or 3 mutations in the central region. In contrast, the vif sequence, which was conserved across clades except for single mutations at positions 14 and 17, inhibited viruses from 5 different clades. Moreover, siRNAs with introduced mutations at sites of gag sequence polymorphisms showed reduced antiviral activity, whereas mutations in vif siRNA only modestly decreased silencing. Thus, although 1 or 2 mutations at peripheral sites are tolerated, mutations in the central target cleavage region abolish RNAi activity.

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Year:  2005        PMID: 15831707      PMCID: PMC1895148          DOI: 10.1182/blood-2004-10-3959

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  49 in total

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3.  Tolerance for mutations and chemical modifications in a siRNA.

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Review 4.  siRNAs, ribozymes and RNA decoys in modeling stem cell-based gene therapy for HIV/AIDS.

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5.  A lentivirus-based system to functionally silence genes in primary mammalian cells, stem cells and transgenic mice by RNA interference.

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9.  Sustained small interfering RNA-mediated human immunodeficiency virus type 1 inhibition in primary macrophages.

Authors:  Erwei Song; Sang-Kyung Lee; Derek M Dykxhoorn; Carl Novina; Dong Zhang; Keith Crawford; Jan Cerny; Phillip A Sharp; Judy Lieberman; N Manjunath; Premlata Shankar
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Review 10.  Interfering with disease: opportunities and roadblocks to harnessing RNA interference.

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  51 in total

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Authors:  Priya S Shah; Nhung P Pham; David V Schaffer
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3.  Determinants of specific RNA interference-mediated silencing of human beta-globin alleles differing by a single nucleotide polymorphism.

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4.  Sequence homology required by human immunodeficiency virus type 1 to escape from short interfering RNAs.

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5.  Production of highly potent recombinant siRNAs in Escherichia coli.

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Review 6.  Selection of RNAi-based inhibitors for anti-HIV gene therapy.

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7.  Inhibition of HIV transmission in human cervicovaginal explants and humanized mice using CD4 aptamer-siRNA chimeras.

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8.  HIV evades RNA interference directed at TAR by an indirect compensatory mechanism.

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10.  A novel approach for inhibition of HIV-1 by RNA interference: counteracting viral escape with a second generation of siRNAs.

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