ZGLP1 is a determinant for the oogenic fate in mice

Nagaoka So I.; Nakaki Fumio; Miyauchi Hidetaka; Nosaka Yoshiaki; Ohta Hiroshi; Yabuta Yukihiro; Kurimoto Kazuki; Hayashi Katsuhiko; Nakamura Tomonori; Yamamoto Takuya; Saitou Mitinori

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ZGLP1 is a determinant for the oogenic fate in mice

机译：ZGLP1是小鼠中源性命运的决定因素

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Sex determination of germ cells is vital to creating the sexual dichotomy of germ cell development, thereby ensuring sexual reproduction. However, the underlying mechanisms remain unclear. Here, we show that ZGLP1, a conserved transcriptional regulator with GATA-like zinc fingers, determines the oogenic fate inmice. ZGLP1 acts downstream of bone morphogenetic protein, but not retinoic acid (RA), and is essential for the oogenic program and meiotic entry. ZGLP1 overexpression induces differentiation of in vitro primordial germ cell-like cells (PGCLCs) into fetal oocytes by activating the oogenic programs repressed by Polycomb activities, whereas RA signaling contributes to oogenic program maturation and PGC program repression. Our findings elucidate the mechanism for mammalian oogenic fate determination, providing a foundation for promoting in vitro gametogenesis and reproductive medicine.

机译：性毒细胞的性别测定对于产生生殖细胞发展的性二分法至关重要，从而确保性繁殖。但是，潜在机制仍然不清楚。在这里，我们表明ZGLP1是一种带有Gata样锌手指的保守转录调节剂，决定了ofogencic命运inmice。 ZGLP1作用在骨形态发生蛋白的下游，但不是视黄酸（RA），并且对于ofocal程序和减数分裂的必不可少。 ZgLP1过度表达通过激活多群活动抑制的归因地，诱导体外原始生殖细胞样细胞（PGCLC）分化成胎儿卵母细胞，而RA信号传导有助于造成ofogencic程序成熟和PGC计划抑制。我们的研究结果阐明了哺乳动物致癌物理测定的机制，为促进体外配子生成和生殖医学提供了基础。

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《Science》 |2020年第6482期|1O89-1089|共2页
作者
Nagaoka So I.; Nakaki Fumio; Miyauchi Hidetaka; Nosaka Yoshiaki; Ohta Hiroshi; Yabuta Yukihiro; Kurimoto Kazuki; Hayashi Katsuhiko; Nakamura Tomonori; Yamamoto Takuya; Saitou Mitinori;
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Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan;

Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|European Mol Biol Lab EMBL Barcelona Multicellular Syst Biol Grp Barcelona 08003 Spain;

Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Div Hepatobiliary Pancreat Surg & Transplantat Dept Surg Kyoto 6068507 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan;

Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Nara Med Univ Dept Embryol Nara 6348521 Japan;

Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyushu Univ Dept Dev Stem Cell Biol Fac Med Sci Fukuoka 8128582 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Ctr iPS Cell Res & Applicat CiRA Sakyo Ku 53 Kawahara Cho Kyoto 6068507 Japan|AMED CREST Chiyoda Ku 1-7-1 Otemachi Tokyo 1000004 Japan|RIKEN Ctr Adv Intelligence Project AIP Med Risk Avoidance Based iPS Cells Team Kyoto 6068507 Japan;

Kyoto Univ Inst Adv Study Human Biol ASHBi Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Grad Sch Med Dept Anat & Cell Biol Sakyo Ku Yoshida Konoe Cho Kyoto 6068501 Japan|Kyoto Univ Ctr iPS Cell Res & Applicat CiRA Sakyo Ku 53 Kawahara Cho Kyoto 6068507 Japan;

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收录信息美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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入库时间 2022-08-18 22:15:04

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1. Genomic Analyses of Sperm Fate Regulator Targets Reveal a Common Set of Oogenic mRNAs in Caenorhabditis elegans [J] . Noble Daniel C., Aoki Scott T., Ortiz Marco A., Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation . 2016,第1期

机译：精子命运调节目标的基因组分析揭示了秀丽隐杆线虫的一组常见的成基因mRNA。
2. Genomic Analyses of Sperm Fate Regulator Targets Reveal a Common Set of Oogenic mRNAs in Caenorhabditis elegans [J] . Daniel C. Noble, Jamie M. Verheyden, Judith Kimble, Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation . 2016,第1期

机译：精子命运调节目标的基因组分析揭示了秀丽隐杆线虫的一组常见的成基因mRNA。
3. Expression of cell fate determinants and plastic changes after neurotoxic lesion of adult mice spinal cord by cholera toxin-B saporin. [J] . Gulino R, Perciavalle V, Gulisano M The European Journal of Neuroscience . 2010,第8期

机译：霍乱毒素-B Saporin对成年小鼠脊髓神经毒性损伤后细胞命运决定因子的表达和塑性变化。
4. Evaluation of the in vivo fate of ultrapure alginate in mice model [C] . A Anitha, Nicholas Fletcher, Zachary Houston, World biomaterials congress . 2016

机译：超纯藻酸盐在小鼠模型中的体内命运评估
5. Filomicelles Deliver a Chemo-Differentiative Therapy to Durably Control Carcinoma Cell Fate [D] . Nair, Praful Raveendran. 2017

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6. Genomic Analyses of Sperm Fate Regulator Targets Reveal a Common Set of Oogenic mRNAs in Caenorhabditis elegans [O] . Daniel C. Noble, Scott T. Aoki, Marco A. Ortiz, 2016

机译：精子命运调节目标的基因组分析揭示了秀丽隐杆线虫的一组常见的成基因mRNA。
7. ZGLP1 is a determinant for the oogenic fate in mice [O] . So I. Nagaoka, Fumio Nakaki, Hidetaka Miyauchi, 2020

机译：ZGLP1是小鼠中源性命运的决定因素
8. IgD Allotypic Determinants. II. Determinants Expressed on IgD of Mice of the B, E, and O Igh-C Haplotypes [R] . Woods, V. L., Scher, I., Lieberman, R., 1980

机译：IgD同种异型决定因素。 II。对B，E和O Igh-C单倍型小鼠的IgD表达的决定因素

ZGLP1 is a determinant for the oogenic fate in mice

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