A DNA vector-based RNAi technology to suppress gene expression in mammalian cells

Sui, Guangchao; Soohoo, Christina; Affar, El Bachir; Gay, Frédérique; Shi, Yujiang Geno; Forrester, William C.; Shi, Yang

doi:10.1073/pnas.082117599

Cited by 1,043 publications

(755 citation statements)

References 21 publications

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“…35 Three siRNA sequences from various coding regions of human Apollon gene were selected (Figure 1b). To generate an intermediate plasmid for cloning shRNAs targeted to Apollon, the oligonucleotide 5 0 -GGCCAGTATGGCTTGCTAGTA-3 0 annealed with the oligonucleotide 5 0 -AGCTTACTAGCAAGCCA TACTGGCC-3 0 was inserted into the ApaI (blunted) and HindIII sites of pBS/U6.…”

Section: Plasmid Vectorsmentioning

confidence: 99%

Oncolytic adenovirus-mediated shRNA against Apollon inhibits tumor cell growth and enhances antitumor effect of 5-fluorouracil

Chu

Sun

et al. 2008

Gene Ther

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Apollon, a membrane-associated inhibitor of apoptosis protein, protects cells against apoptosis and is upregulated in certain tumor cells. In this study, the effects of Apollon protein knockdown by RNA interference on the growth of human HeLa, HT-1080 and MCF-7 cells in vitro and in vivo were investigated. An oncolytic adenovirus (ZD55) containing the RNA polymerase III-dependent U6 promoter to express short hairpin RNA (shRNA) directed against Apollon (ZD55-siApollon) was constructed. Our data show that ZD55-siApollon successfully exerts a gene knockdown effect and causes the inhibition of tumor cell growth both in culture and in athymic mice in vivo. Cell cycle analysis, 4 0 ,6-diamidino-2-phenylindole staining and western blot analysis reveal that ZD55-siApollon-mediated suppression of Apollon induces apoptosis. Intratumoral injection of ZD55-siApollon significantly inhibits tumor growth in HT-1080 xenograft mice. Furthermore, ZD55-siApollon enhances the antitumor effect of 5-fluorouracil, a chemotherapeutic agent. In conclusion, these results suggest that the depletion of Apollon by oncolytic adenovirus-shRNA delivery system provides a promising method for cancer therapy.

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Section: Plasmid Vectorsmentioning

confidence: 99%

Oncolytic adenovirus-mediated shRNA against Apollon inhibits tumor cell growth and enhances antitumor effect of 5-fluorouracil

Chu

Sun

et al. 2008

Gene Ther

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“…Numerous additional reports indicate that certain individuals or groups are immune to HIV-1 altogether (Baur et al 1989, Bryson et al 1995, Deacon et al 1995, Roques et al 1995, Paxton et al 1996, Kaul et al 2000, Kulkarni et al 2003, while others remain AIDS free for extensive periods of time . In order to develop sufficient human protection against HIV-1 variants, a number of homologous sequences will be required in the endogenous repertoire (Hiroshika et al 2000, Donze & Picard 2002, Hohjoh 2002, Jeong et al 2002, Leirdal & Sioud 2002, Miyagishi & Taira 2002, Paddison et al 2002, Paul et al 2002, Sui et al 2002, Yu et al 2002. Through genetic technology, however, a rapid HIV-1 inhibitory siRNAs specific repertoire can perhaps be designed.…”

Section: Role Of Sirnas In Development Of Hiv-1 Vaccinementioning

confidence: 99%

“…Through genetic technology, however, a rapid HIV-1 inhibitory siRNAs specific repertoire can perhaps be designed. These siRNAs could be encoded and delivered by appropriate vectors and then utilized in preventative or therapeutic vaccines (Hiroshika et al 2000, Donze & Picard 2002, Hohjoh 2002, Jeong et al 2002, Leirdal & Sioud 2002, Miyagishi & Taira 2002, Paddison et al 2002, Paul et al 2002, Sui et al 2002, Yu et al 2002.…”

Section: Role Of Sirnas In Development Of Hiv-1 Vaccinementioning

confidence: 99%

“…One way to answer this question is to evaluate what happens to an organism when certain genes, presumed to be involved in RBGS, are altered. Mutations in several genes render an organism incapable of generating siRNAs; in some cases, these mutations reactivate transposons and retroelements (Ketting et al 1999, Tabara et al 1999, Hirochika et al 2000, Nakayashiki et al 2001, Jeong et al 2002, Paddison et al 2002, Paul et al 2002, Sui et al 2002. Proteins essential for the homologous RNA degradation pathway are highly conserved in fungi, plants, vertebrates, and mammals (reviewed in Grishok & Mello 2002).…”

Section: Issues With Current Models Of Rnaimentioning

confidence: 99%

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RNA interference: The molecular immune system

Bagasra

Prilliman²

2004

Histochem J

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SummaryIntroduction of double-stranded RNA (dsRNA) into cells expressing a homologous gene triggers RNA interference (RNAi), or RNA-based gene silencing (RBGS). The dsRNA degrades corresponding host mRNA into small interfering RNAs (siRNAs) by a protein complex containing Dicer. siRNAs in turn are incorporated into the RNA-induced silencing complex (RISC) that includes helicase, RecA, and exo-and endo-nucleases as well as other proteins. Following its assembly, the RISC guides the RNA degradation machinery to the target RNAs and cleaves the cognate target RNA in a sequence-specific, siRNA-dependent manner. RNAi has now been documented in a wide variety of organisms, including plants, fungi, flies, worms, and more recently, higher mammals. In eukaryotes, dsRNA directed against a range of viruses (i.e., HIV-1, RSV, HPV, poliovirus and others) and endogenous genes can induce sequence-specific inhibition of gene expression. In invertebrates, RNAi can be efficiently triggered by either long dsRNAs or 21-to 23-nt-long siRNAs. However, in jawed vertebrates, dsRNA longer than 30 bp can induce interferon and thus trigger undesirable side effects instead of initiating RNAi. siRNAs have been shown to act as potent inducers of RNAi in cultured mammalian cells. Many investigators have suggested that siRNAs may have evolved as a normal defense against endogenous and exogenous transposons and retroelements. Through a combination of genetic and biochemical approaches, some of the mechanisms underlying RNAi have been described. Recent data in C. elegans shows that two homologs of siRNAs, microRNAs (miRNAs) and tiny noncoding RNAs (tncRNAs) are endogenously expressed. However, many aspects of RNAi-induced gene silencing, including its origins and the selective pressures which maintain it, remain undefined. Its evolutionary history may pass through the more primitive immune functions of prokaryotes involving restriction enzymes that degrade plasmid DNA molecules that enter bacterial cells. RNAi has evolved further among eukaryotes, in which its wide distribution suggests early origins. RNAi seems to be involved in a variety of regulatory and immune functions that may differ among various kingdoms and phyla. We present here proposed mechanisms by which RBGS protects the host against endogenous and exogenous transposons and retroelements. The potential for therapeutic application of RBGS technology in treating viral infections such as HIV is also discussed.

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“…Thus Pol III transcripts normally have 3-4 U residues at the 3 0 end (for a review see Schramm and Hernandez 21 ). A flurry of papers in 2002 from five different groups [22][23][24][25][26] established that short hairpin RNA (shRNA) molecules expressed from U6 or H1 Type 3 Pol III promoters could mediate sequence-specific RNAi-based gene inhibition. All of the groups designed expression units where the RNA sequence expressed from the Pol III promoters contained an inverted repeat of 19-29 nt separated by a short spacer sequence (See Figure 1a).…”

Section: Codon Optimization and Codon Pairing Will Affect Transcriptimentioning

confidence: 99%

Gene Therapy Progress and Prospects: Recent progress in transgene and RNAi expression cassettes

Ill¹,

Chiou²

2005

Gene Ther

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Plasmid expression cassette design must include a thoughtful analysis of potentially every nucleotide comprising a covalently closed circular or end-protected linear DNA. This review will discuss recent studies in unraveling the mechanisms of postdelivery gene silencing, codon optimization and promoter identification. The recent discovery of potent RNA interference (RNAi) mechanisms for sequence-specific gene silencing has also invoked a great deal of interest in development of expression cassettes that can produce double-stranded RNA molecules for RNAi. Expression cassettes based on both RNA polymerase II and polymerase III transcription units that generate double-stranded RNA molecules for RNAi will also be discussed. Gene Therapy (2005) Whether a mammalian cell expression cassette is produced by bacterial amplification, minicircle recombination, or by purely synthetic means, the primary DNA

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A DNA vector-based RNAi technology to suppress gene expression in mammalian cells

Cited by 1,043 publications

References 21 publications

Oncolytic adenovirus-mediated shRNA against Apollon inhibits tumor cell growth and enhances antitumor effect of 5-fluorouracil

Oncolytic adenovirus-mediated shRNA against Apollon inhibits tumor cell growth and enhances antitumor effect of 5-fluorouracil

RNA interference: The molecular immune system

Gene Therapy Progress and Prospects: Recent progress in transgene and RNAi expression cassettes

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