Distinct Imprinting Signatures and Biased Differentiation of Human Androgenetic and Parthenogenetic Embryonic Stem Cells

Sagi, Ido; Pinho, Joao Correia De; Zuccaro, Michael V.; Atzmon, Chen; Golan‐Lev, Tamar; Yanuka, Ofra; Prosser, Robert; Sadowy, Alexandra; Perez, Gloria I.; Cabral, Thiago; Gläser, Benjamin; Tsang, Stephen H.; Goland, Robin; Sauer, Mark V.; Løbo, Rogerio A.; Benvenisty, Nissim; Egli, Dieter

doi:10.1016/j.stem.2019.06.013

Cited by 31 publications

(43 citation statements)

References 76 publications

(99 reference statements)

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“…In addition, androgenetic embryos that progressed beyond ZGA underwent a second arrest at the morula stage. Similar results have been reported in cattle (Winger et al, 1997; Vichera et al, 2011), sheep (Matsukawa et al, 2007), mouse (Kono et al, 1993; Latham et al, 2002; Hu et al, 2015a; Hu et al, 2015b), and human species (Kuznyetsov et al, 2007; Sagi et al, 2019). Further development to the blastocyst stage, of both haploid parthenotes and androgenotes was severely limited compared to diploid embryos, evidencing a deleterious effect of haploidy on the very early stage of embryogenesis.…”

Section: Discusionsupporting

confidence: 83%

“…In agreement with these findings others have indicated that enucleation during the telophase stage of second meiosis (TII) shows advantages over enucleation at the metaphase II stage. For instance, TII enucleation allows the removal of smaller ooplasm fragments (Bordignon and Smith, 1998; Lee and Campbell, 2006), can be performed in the absence of UV irradiation (Kuznyetsov et al, 2007; Sagi et al, 2019), and it also allows the selection of the best oocytes for enucleation through the exclusive use oocytes that respond promptly to fertilization by second polar body extrusion (Kuznyetsov et al, 2007).…”

Section: Discusionmentioning

confidence: 99%

“…However, in bovine species the efforts to visualize and enucleate zygotes at pronuclear stages is hampered by the presence of dense lipid vesicles, and thus, usually, removal of the oocytes metaphase spindle is performed pre-IVF, as in the case of SCNT, at approximately 18 to 20 h after beginning of in vitro maturation (MII enucleation). Otherwise, during the telophase to anaphase transition of meiosis II the second polar body is a reliable indicator of the position of the oocyte’s spindle and it can be reliably used to enucleate mammalian oocytes (Bordignon and Smith, 1998; Kuznyetsov et al, 2007; Sagi et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

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Dysregulated gene expression of imprinted and X-linked genes: a link to poor development of bovine haploid androgenetic embryos

Águila

Therrien

Suzuki

et al. 2020

Preprint

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Mammalian uniparental embryos are efficient models for genome imprinting research and allow studies on the contribution of the paternal and maternal genome to early embryonic development. In this study, we analyzed different methodologies for production of bovine haploid androgenetic embryos (hAE) to elucidate the causes behind their poor developmental potential. The results showed that hAE can be efficiently generated by using intracytoplasmic sperm injection and oocyte enucleation at telophase II. Although haploidy does not disturb early development up to around the 3rd mitotic division, androgenetic development is disturbed after the time of zygote genome activation those that reach the morula stage are less capable to become a blastocyst. Analysis of gene expression indicated abnormal levels of methyltransferase 3B and key long non-coding RNAs involved in X-chromosome inactivation and genomic imprinting of the KCNQ1 locus, which is associated to the methylation status of imprinted control regions of XIST and KCNQ1OT1. Thus, our results seem to exclude micromanipulation consequences and chromosomal abnormalities as major factors in developmental restriction, suggesting that their early developmental constraint is regulated at an epigenetic level.

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Section: Discusionsupporting

confidence: 83%

Section: Discusionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Dysregulated gene expression of imprinted and X-linked genes: a link to poor development of bovine haploid androgenetic embryos

Águila

Therrien

Suzuki

et al. 2020

Preprint

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show abstract

“…As mentioned above, monoallelic knockout animal models carrying heritable lethal mutations could be generated efficiently in the F0 generation, while this is not achievable by traditional methods 18 . As several recent studies have revealed, abundant parental-specific gene expression exerts a great influence on pre-or post-implantation development, but diseases resulting from these early changes are difficult to ascertain due to the unobservable symptom in early stages of pregnancy 24,50,51 . However, Past-CRISPR has great advantages in terms of the functional verification of individual parent-of-origin genes, including imprinted gene candidates.…”

Section: Discussionmentioning

confidence: 99%

Precise allele-specific genome editing by spatiotemporal control of CRISPR-Cas9 via pronuclear transplantation

Weng

Bai

et al. 2020

Nat Commun

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Gene-targeted animal models that are generated by injecting Cas9 and sgRNAs into zygotes are often accompanied by undesired double-strand break (DSB)-induced byproducts and random biallelic targeting due to uncontrollable Cas9 targeting activity. Here, we establish a parental allele-specific gene-targeting (Past-CRISPR) method, based on the detailed observation that pronuclear transfer-mediated cytoplasmic dilution can effectively terminate Cas9 activity. We apply this method in embryos to efficiently target the given parental alleles of a gene of interest and observed little genomic mosaicism because of the spatiotemporal control of Cas9 activity. This method allows us to rapidly explore the function of individual parent-of-origin effects and to construct animal models with a single genomic change. More importantly, Past-CRISPR could also be used for therapeutic applications or disease model construction.

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“…In mammals, both parents make unique contributions to the offspring and maternal and paternal genomes are required for development. Two recent papers in Cell Stem Cell (Leng et al, 2019;Sagi et al, 2019) study uniparental embryos and uniparental embryonic stem cells to interrogate parent-of-origin effects in human embryogenesis.…”

mentioning

confidence: 99%

From Mother or Father: Uniparental Embryos Uncover Parent-of-Origin Effects in Humans

Aizawa

Wutz

2019

Cell Stem Cell

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Distinct Imprinting Signatures and Biased Differentiation of Human Androgenetic and Parthenogenetic Embryonic Stem Cells

Cited by 31 publications

References 76 publications

Dysregulated gene expression of imprinted and X-linked genes: a link to poor development of bovine haploid androgenetic embryos

Dysregulated gene expression of imprinted and X-linked genes: a link to poor development of bovine haploid androgenetic embryos

Precise allele-specific genome editing by spatiotemporal control of CRISPR-Cas9 via pronuclear transplantation

From Mother or Father: Uniparental Embryos Uncover Parent-of-Origin Effects in Humans

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