Long-term, efficient inhibition of microRNA function in mice using rAAV vectors

Xie, Jun; Ameres, Stefan L.; Friedline, Randall H.; Hung, Jui-Hung; Zhang, Yu; Xie, Qing; Zhong, Li; Su, Qin; He, Ran; Li, Mengxin; Li, Huapeng; Mu, Xin; Zhang, Hongwei; Broderick, Jennifer A.; Kim, Jason K.; Weng, Zhiping; Flotte, Terence R.; Zamore, Phillip D.; Gao, Guangping

doi:10.1038/nmeth.1903

Cited by 195 publications

(191 citation statements)

References 30 publications

(41 reference statements)

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“…98 Notably, a novel kind of sponges called anti-miRs is becoming a strong candidate for miRNA-based therapeutics. 43,[99][100][101][102][103][104][105][106][107] The anti-miRs are chemically modified oligonucleotides developed to modulate the activities of specific miRNAs. A recent study carried out by Hogan and his colleagues 108 demonstrated that the anti-miR physically associated with the AGO protein complex in the context of the cognate target miRNA both in vitro and in vivo.…”

Section: Degradome-seqmentioning

confidence: 99%

The use of high-throughput sequencing methods for plant microRNA research

Tang

Qin³

et al. 2015

RNA Biology

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Section: Degradome-seqmentioning

confidence: 99%

The use of high-throughput sequencing methods for plant microRNA research

Tang

Qin³

et al. 2015

RNA Biology

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“…Such adaptations of the miRNA sponge concept allow longer-term inhibition of miRNAs than can be achieved by transient transfection of RNA polymerase II sponge reporter vectors or modified RNA oligonucleotides. Xie et al (2012) combined recombinant adeno-associated virus (rAAV) vectors with miRNA TuDs to inhibit specific miRNAs. Injection of a rAAV9 construct expressing anti-miR-122 or anti-let-7 TuDs resulted in long-term depletion of the corresponding miRNA and increased expression of its mRNA targets.…”

Section: Mirna Sponges/decoysmentioning

confidence: 99%

Strategies to deliver microRNAs as potential therapeutics in the treatment of cardiovascular pathology

2012

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“…Studies have also shown that RNA polymerase II promoters can be used to efficiently express TuD inhibitors within the cell [24,25]. It has been shown that adeno-associated virus-delivered TuDs induced long-term miRNA inhibition in mice [27,28]. TuDs and sponges are both more effective when the miRNA binding sites are non-complementary to the target miRNA at position 10–11, presumably because Ago2-dependent cleavage of the TuD is prevented [23,25,29].…”

Section: Introductionmentioning

confidence: 99%

“…TuDs and sponges are both more effective when the miRNA binding sites are non-complementary to the target miRNA at position 10–11, presumably because Ago2-dependent cleavage of the TuD is prevented [23,25,29]. Whether TuD activity is mediated by miRNA sequestration alone, or also by miRNA degradation remains unclear, since several studies have reported conflicting results [20,23,27]. In comparative studies, TuDs proved more effective miRNA inhibitors than sponges [23,27].…”

Section: Introductionmentioning

confidence: 99%

“…Whether TuD activity is mediated by miRNA sequestration alone, or also by miRNA degradation remains unclear, since several studies have reported conflicting results [20,23,27]. In comparative studies, TuDs proved more effective miRNA inhibitors than sponges [23,27]. Recently, an AAV-based TuD has been successfully used to restore cardiac function in a murine heart failure model by targeting miR-25 [28].…”

Section: Introductionmentioning

confidence: 99%

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RNA accessibility impacts potency of Tough Decoy microRNA inhibitors

et al. 2018

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MicroRNAs (miRNAs) are small RNA molecules that post-transcriptionally regulate gene expression through silencing of complementary target mRNAs. miRNAs are involved in many biological processes, including cell proliferation, differentiation, cell signaling and cellular defense responses to infection. Strategies that allow for strong and stable suppression of specific microRNA activity are needed to study miRNA functions and to develop therapeutic intervention strategies aimed at interfering with miRNA activity in vivo. One of these classes of miRNA inhibitors are Tough Decoys (TuD) RNAs, which comprise of an imperfect RNA hairpin structure that harbors two opposing miRNA binding sites. Upon developing TuDs targeting Epstein-Barr virus miRNAs, we observed a strong variation in inhibitory potential between different TuD RNAs targeting the same miRNA. We show that the composition of the ‘bulge’ sequence in the miRNA binding sites has a strong impact on the inhibitory potency of the TuD. Our data implies that miRNA inhibition correlates with the thermodynamic properties of the TuD and that design aimed at lowering the TuD opening energy increases TuD potency. Our study provides specific guidelines for the design and construction of potent decoy-based miRNA inhibitors, which may be used for future therapeutic intervention strategies.

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Long-term, efficient inhibition of microRNA function in mice using rAAV vectors

Cited by 195 publications

References 30 publications

The use of high-throughput sequencing methods for plant microRNA research

The use of high-throughput sequencing methods for plant microRNA research

Strategies to deliver microRNAs as potential therapeutics in the treatment of cardiovascular pathology

RNA accessibility impacts potency of Tough Decoy microRNA inhibitors

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