Nonviral Gene Delivery with the <i>Sleeping Beauty</i> Transposon System

Ivics, Zoltán; Izsvák, Zsuzsanna

doi:10.1089/hum.2011.143

Cited by 59 publications

(42 citation statements)

References 89 publications

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“…The first clinical application of the SB system will help to validate both the safety and efficacy of this approach. Applications of the SB system fall outside the scope of this chapter, and readers are referred to recent review articles (160,161,162,163,164,165,166,167,168,169,170,171,172).…”

Section: Sleeping Beauty As a Genetic Toolmentioning

confidence: 99%

Sleeping Beauty Transposition

Ivics

Izsvák

2015

Microbiol Spectr

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Sleeping Beauty (SB) is a synthetic transposon that was constructed based on sequences of transpositionally inactive elements isolated from fish genomes. SB is a Tc1/mariner superfamily transposon following a cut-and-paste transpositional reaction, during which the element-encoded transposase interacts with its binding sites in the terminal inverted repeats of the transposon, promotes the assembly of a synaptic complex, catalyzes excision of the element out of its donor site, and integrates the excised transposon into a new location in target DNA. SB transposition is dependent on cellular host factors. Transcriptional control of transposase expression is regulated by the HMG2L1 transcription factor. Synaptic complex assembly is promoted by the HMGB1 protein and regulated by chromatin structure. SB transposition is highly dependent on the nonhomologous end joining (NHEJ) pathway of double-strand DNA break repair that generates a transposon footprint at the excision site. Through its association with the Miz-1 transcription factor, the SB transposase downregulates cyclin D1 expression that results in a slowdown of the cell-cycle in the G1 phase, where NHEJ is preferentially active. Transposon integration occurs at TA dinucleotides in the target DNA, which are duplicated at the flanks of the integrated transposon.

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Section: Sleeping Beauty As a Genetic Toolmentioning

confidence: 99%

Sleeping Beauty Transposition

Ivics

Izsvák

2015

Microbiol Spectr

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“…Up to 900 genes may be modified by lentiviral infection of CD34 + cells [32]. These problems ask for special safety regards before lentiviral vectors can proceed to the clinic [33] or, for example, the use of nonviral gene delivery systems, such as the ''sleeping beauty,'' may be advisable [34]. In spite of all these caveats, it has been documented that in vitro and even in vivo lentiviral infection of MSCs did not affect their multilineage differentiation potential [35] and in our case, tenogenic tissue formation of control implantations with GFP-lentiviruses or uninfected MSCs was not observed (data not shown).…”

Section: Periostin and Tumorigenesismentioning

confidence: 99%

Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

Noack

Seiffart

Willbold

et al. 2014

Stem Cells and Development

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True tendon regeneration in human patients remains a vision of musculoskeletal therapies. In comparison to other mesenchymal lineages the biology of tenogenic differentiation is barely understood. Specifically, easy and efficient protocols are lacking that might enable tendon cell and tissue differentiation based on adult (stem) cell sources. In the murine mesenchymal progenitor cell line C3H10T½, overexpression of the growth factor bone morphogenetic protein 2 (BMP2) and a constitutively active transcription factor, Smad8 L + MH2, mediates tendon cell differentiation in vitro and the formation of tendon-like tissue in vivo. We hypothesized that during this differentiation secreted factors involved in extracellular matrix formation exert a major impact on tendon development. Gene expression analyses revealed four genes encoding secreted factors that are notably upregulated: periostin, C-type lectin domain family 3 (member b), RNase A4, and follistatin-like 1. These factors have not previously been implicated in tendon biology. Among these, periostin showed a specific expression in tenocytes of adult mouse Achilles tendon and in chondrocytes within the nonmineralized fibrocartilage zone of the enthesis with the calcaneus. Overexpression of periostin alone or in combination with constitutively active BMP receptor type in human mesenchymal stem cells and subsequent implantation into ectopic sites in mice demonstrated a reproducible moderate tenogenic capacity that has not been described before. Therefore, periostin may belong to the factors contributing to the development of tenogenic tissue.

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“…By exploiting the local hopping feature of the SB system, it was possible to decipher the genomic neighborhood of a particular integration site by remobilizing the transposons from individual chromosomes (Keng et al, 2005;Kokubu et al, 2009). The greatest success of SB has been in its use for phenotype-driven genetics (Carlson et al, 2003;Elso et al, 2015;Horie et al, 2003;Ivics & Izsvak, 2011;Izsvak et al, 2010;Moriarity & Largaespada, 2011). Unlike a candidate-based strategy, SB transposon-based gene trapping, enhancer trapping and unbiased mutagenesis approach is suitable to identify genes with unexpected phenotypes (Balciunas et al, 2004;Lu et al, 2007;Song & Cui, 2013).…”

Section: Awakening Sleeping Beauty In the Clinicmentioning

confidence: 99%

Sleeping Beautytransposition: from biology to applications

Narayanavari

Chilkunda

Ivics

et al. 2016

Critical Reviews in Biochemistry and Molecular Biology

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Sleeping Beauty (SB) is the first synthetic DNA transposon that was shown to be active in a wide variety of species. Here, we review studies from the last two decades addressing both basic biology and applications of this transposon. We discuss how host-transposon interaction modulates transposition at different steps of the transposition reaction. We also discuss how the transposon was translated for gene delivery and gene discovery purposes. We critically review the system in clinical, pre-clinical and non-clinical settings as a non-viral gene delivery tool in comparison with viral technologies. We also discuss emerging SB-based hybrid vectors aimed at combining the attractive safety features of the transposon with effective viral delivery. The success of the SBbased technology can be fundamentally attributed to being able to insert fairly randomly into genomic regions that allow stable long-term expression of the delivered transgene cassette. SB has emerged as an efficient and economical toolkit for safe and efficient gene delivery for medical applications.ARTICLE HISTORY

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Nonviral Gene Delivery with the Sleeping Beauty Transposon System

Cited by 59 publications

References 89 publications

Sleeping Beauty Transposition

Sleeping Beauty Transposition

Periostin Secreted by Mesenchymal Stem Cells Supports Tendon Formation in an Ectopic Mouse Model

Sleeping Beautytransposition: from biology to applications

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