Specification and epigenetic resetting of the pig germline exhibit conservation with the human lineage

Zhu, Qifan; Sang, Fei; Withey, Sarah; Tang, Walfred W.C.; Dietmann, Sabine; Klisch, Doris; Ramos‐Ibeas, Priscila; Zhang, Haixin; Requena, Cristina E.; Hájková, Petra; Loose, Matt; Surani, M. Azim; Alberio, Ramiro

doi:10.1101/2020.08.07.241075

Cited by 3 publications

(14 citation statements)

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“…Recent work from our laboratories has shown the developmental correspondence between human and pig germ cells during the initial period of gastrulation (Kobayashi et al, 2017;Zhu et al, 2021). We propose that building on these investigations into pig gastrulation using singlecell -omics and gene manipulation will offer new knowledge on the mechanisms of meso-endoderm and ectoderm specification with relevance to understanding human development.…”

Section: Reviewmentioning

confidence: 95%

“…Notably, pig PGCs are first found in the posterior epiblast expressing SOX17, BLIMP1, and TFAP2C, and the cluster expands to about 120 cells by induction of proliferating PGC-competent progenitors upon exposure to BMP. These newly formed pig PGCs (pPGCs) pause their proliferation briefly, only to resume cell-cycle progression after they start their migration (Kobayashi et al, 2017;Zhu et al, 2021). The PGCs originating in the amnion of Cynomolgus monkey appear to be in a proliferative phase soon after specification (Sasaki et al, 2016), but how PGCs migrate to posterior epiblast against the movement of amnion that expands toward the opposite direction merits further investigations.…”

Section: Origin Of the Germline In Mammalsmentioning

confidence: 99%

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Conserved features of non-primate bilaminar disc embryos and the germline

2021

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Post-implantation embryo development commences with a bilaminar disc in most mammals, including humans. Whereas access to early human embryos is limited and subject to greater ethical scrutiny, studies on non-primate embryos developing as bilaminar discs offer exceptional opportunities for advances in gastrulation, the germline, and the basis for evolutionary divergence applicable to human development. Here, we discuss the advantages of investigations in the pig embryo as an exemplar of development of a bilaminar disc embryo with relevance to early human development. Besides, the pig has the potential for the creation of humanized organs for xenotransplantation. Precise genetic engineering approaches, imaging, and single-cell analysis are cost effective and efficient, enabling research into some outstanding questions on human development and for developing authentic models of early human development with stem cells.

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Section: Reviewmentioning

confidence: 95%

Section: Origin Of the Germline In Mammalsmentioning

confidence: 99%

Conserved features of non-primate bilaminar disc embryos and the germline

2021

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“…More recently, it has been shown that PRDM14 mediates the removal of H3K27me3 marks from the Xi during XCR in PGCs [ 143 ]. In addition, a recent study in pig showed that Xist is silenced in most pre-migratory PGCs [ 144 ]. XCR begins in pre/early migrating PGCs and continues in gonadal PGCs.…”

Section: Xcr During Mouse Developmentmentioning

confidence: 99%

“…XCR begins in pre/early migrating PGCs and continues in gonadal PGCs. The kinetics of XCR is not explained by distance of genes to the Xic [ 144 ]. In summary, XCR takes places during epigenetic reprogramming of the germline and is linked to the expression of pluripotency genes, including transcription factors.…”

Section: Xcr During Mouse Developmentmentioning

confidence: 99%

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New Insights into X-Chromosome Reactivation during Reprogramming to Pluripotency

Panda

Ż̷ylicz

Pasque

2020

Cells

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Dosage compensation between the sexes results in one X chromosome being inactivated during female mammalian development. Chromosome-wide transcriptional silencing from the inactive X chromosome (Xi) in mammalian cells is erased in a process termed X-chromosome reactivation (XCR), which has emerged as a paradigm for studying the reversal of chromatin silencing. XCR is linked with germline development and induction of naive pluripotency in the epiblast, and also takes place upon reprogramming somatic cells to induced pluripotency. XCR depends on silencing of the long non-coding RNA (lncRNA) X inactive specific transcript (Xist) and is linked with the erasure of chromatin silencing. Over the past years, the advent of transcriptomics and epigenomics has provided new insights into the transcriptional and chromatin dynamics with which XCR takes place. However, multiple questions remain unanswered about how chromatin and transcription related processes enable XCR. Here, we review recent work on establishing the transcriptional and chromatin kinetics of XCR, as well as discuss a model by which transcription factors mediate XCR not only via Xist repression, but also by direct targeting of X-linked genes.

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Generation of germ cell-deficient pigs by <i>NANOS3</i> knockout

Kogasaka

Murakami

Yamashita

et al. 2022

Journal of Reproduction and Development

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NANOS3 is an evolutionarily conserved gene expressed in primordial germ cells that is important for germ cell development. Germ cell deletion by NANOS3 knockout has been reported in several mammalian species, but its function in pigs is unclear. In the present study, we investigated the germline effects of NANOS3 knockout in pigs using CRISPR/Cas9. Embryo transfer of CRISPR/Cas9modified embryos produced ten offspring, of which one showed wild-type NANOS3 alleles, eight had two mutant NANOS3 alleles, and the other exhibited mosaicism (four mutant alleles). Histological analysis revealed no germ cells in the testes or ovaries of any of the nine mutant pigs. These results demonstrated that NANOS3 is crucial for porcine germ cell production.

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Specification and epigenetic resetting of the pig germline exhibit conservation with the human lineage

Cited by 3 publications

References 86 publications

Conserved features of non-primate bilaminar disc embryos and the germline

Conserved features of non-primate bilaminar disc embryos and the germline

New Insights into X-Chromosome Reactivation during Reprogramming to Pluripotency

Generation of germ cell-deficient pigs by <i>NANOS3</i> knockout

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