Transient Dux expression facilitates nuclear transfer and induced pluripotent stem cell reprogramming

Yang, Lei; Liu, Xuefei; Song, Lishuang; Di, Anqi; Su, Guanghua; Bai, Chunling; Wei, Zhuying; Li, Guangpeng

doi:10.15252/embr.202050054

Cited by 31 publications

(34 citation statements)

References 56 publications

(77 reference statements)

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“…Resent research has also demonstrated that the ectopic expression of DUX alone in mouse embryonic stem cells can activate MERVL, accompanied by a "two-cell-like" transcriptional program, which often corresponds with ZGA [27,29]. Indeed, transient overexpression of DUX can significantly increase the expression of MERVL, indicating that DUX acts as a core factor for ZGA by enhancing the expression of ZGA-specific genes such as Zscan4, Zfp352, and MERVL [72,73]. Given the versatility of ERVs, it seems likely that ancestral DUX proteins strengthened their control over the ZGA process by regulating ERVs [28].…”

Section: Erv Activation During Zgamentioning

confidence: 99%

“…Because the timely expression of ZGA is indispensable for the development of cloned embryos, and DUX, acting as a pioneer transcription factor, can trigger the activation of ERVs and ZGA-specific genes [27][28][29], it is reasonable to suspect that exogenous DUXtreated cloned embryos will acquire higher developmental competence. Yang et al demonstrated that a direct injection of DUX has no significant effect on SCNT blastocyst formation, whereas the transient expression of DUX indeed improves SCNT efficiency, producing a transcriptome profile similar to that of fertilized embryos [73]. The ZGA process is under the control of a "zygotic clock", and the improvement to the efficiency of cloned embryo development induced by DUX is time-dependent.…”

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

“…Conversely, the transient expression of DUX via dox-inducible system during the 11-25 h post-activation period did increase the blastocyst formation rate. Moreover, the transient expression of DUX significantly increased the expression of ZGA-related genes, such as ZSCAN4 and MERVL [73]. The dox-inducible system is a powerful tool for initiating the transient expression of exogenous genes.…”

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

“…This elevated SCNT efficiency benefits from the advantages of the dox-inducible system, which allows the regulation of DUX expression in a spatiotemporal-specific manner via switching between dox-containing and dox-free culture medium, therefore ensuring a timely entry into the ZGA state along with a timely exit from it (Figure 1). cantly increased the expression of ZGA-related genes, such as ZSCAN4 and MERVL [73]. The dox-inducible system is a powerful tool for initiating the transient expression of exogenous genes.…”

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

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Functions and Regulation of Endogenous Retrovirus Elements during Zygotic Genome Activation: Implications for Improving Somatic Cell Nuclear Transfer Efficiency

Liu

2021

Biomolecules

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Endogenous retroviruses (ERVs), previously viewed as deleterious relics of ancestral retrovirus infections, are silenced in the vast majority of cells to minimize the risk of retrotransposition. Counterintuitively, bursts of ERV transcription usually occur during maternal-to-zygotic transition (MZT) in preimplantation embryos; this is regarded as a major landmark event in the zygotic genome activation (ZGA) process, indicating that ERVs play an active part in ZGA. Evolutionarily, the interaction between ERVs and hosts is mutually beneficial. The endogenization of retrovirus sequences rewires the gene regulatory network during ZGA, and ERV repression may lower germline fitness. Unfortunately, owing to various limitations of somatic cell nuclear transfer (SCNT) technology, both developmental arrest and ZGA abnormalities occur in a high percentage of cloned embryos, accompanied by ERV silencing, which may be caused by the activation failure of upstream ERV inducers. In this review, we discuss the functions and regulation of ERVs during the ZGA process and the feasibility of temporal control over ERVs in cloned embryos via exogenous double homeobox (DUX). We hypothesize that further accurate characterization of the ERV-rewired gene regulatory network during ZGA may provide a novel perspective on the development of preimplantation embryos.

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Section: Erv Activation During Zgamentioning

confidence: 99%

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

Section: The Implications Of Ervs Activation For Improving the Developmental Competence Of Cloned Embryosmentioning

confidence: 99%

See 2 more Smart Citations

Functions and Regulation of Endogenous Retrovirus Elements during Zygotic Genome Activation: Implications for Improving Somatic Cell Nuclear Transfer Efficiency

Liu

2021

Biomolecules

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“…Moreover, transcriptome profiling revealed that DUX expressing cloned embryos are similar to fertilized embryos. Furthermore, overexpression of DUX combined with knockdown of DNMTs promoted the full-term of cloned embryos [ 118 ].…”

Section: Specific Attempts To Modulate the Epigenomementioning

confidence: 99%

Manipulating the Epigenome in Nuclear Transfer Cloning: Where, When and How

Simmet

Wolf

Zakhartchenko

2020

IJMS

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The nucleus of a differentiated cell can be reprogrammed to a totipotent state by exposure to the cytoplasm of an enucleated oocyte, and the reconstructed nuclear transfer embryo can give rise to an entire organism. Somatic cell nuclear transfer (SCNT) has important implications in animal biotechnology and provides a unique model for studying epigenetic barriers to successful nuclear reprogramming and for testing novel concepts to overcome them. While initial strategies aimed at modulating the global DNA methylation level and states of various histone protein modifications, recent studies use evidence-based approaches to influence specific epigenetic mechanisms in a targeted manner. In this review, we describe—based on the growing number of reports published during recent decades—in detail where, when, and how manipulations of the epigenome of donor cells and reconstructed SCNT embryos can be performed to optimize the process of molecular reprogramming and the outcome of nuclear transfer cloning.

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Cloning by SCNT: Integrating Technical and Biology-Driven Advances

Moura

2023

Methods in Molecular Biology

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Transient Dux expression facilitates nuclear transfer and induced pluripotent stem cell reprogramming

Cited by 31 publications

References 56 publications

Functions and Regulation of Endogenous Retrovirus Elements during Zygotic Genome Activation: Implications for Improving Somatic Cell Nuclear Transfer Efficiency

Functions and Regulation of Endogenous Retrovirus Elements during Zygotic Genome Activation: Implications for Improving Somatic Cell Nuclear Transfer Efficiency

Manipulating the Epigenome in Nuclear Transfer Cloning: Where, When and How

Cloning by SCNT: Integrating Technical and Biology-Driven Advances

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