Zygotic activin a is dispensable for the mouse preimplantation embryo development and for the derivation and pluripotency of embryonic stem cells†.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2024-11-06 DOI:10.1093/biolre/ioae156
Eliza Winek, Lidia Wolińska-Nizioł, Katarzyna Szczepańska, Anna Szpakowska, Olga Gewartowska, Izabela Wysocka, Magdalena Grzesiak, Aneta Suwińska
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Abstract

In this work, we aimed to determine the role of activin A during crucial events of mouse embryogenesis and distinguish the function of the protein of zygotic origin and the one secreted by the maternal reproductive tract. To this end, we recorded the progression of development and phenotype of Inhba knockout embryos and compared them with the heterozygotes and wild-type embryos using time-lapse imaging and detection of lineage-specific markers. We revealed that the zygotic activin A deficiency does not impair the course and rate of development of embryos to the blastocyst stage. Inhba knockout embryos form functional epiblast, as evidenced by their ability to give rise to embryonic stem cells. Our study is the first to show that derivation, maintenance in culture, and pluripotency of embryo-derived embryonic stem cells are exogenous and endogenous activin A-independent. However, the implantation competence of activin A-deficient embryos may be compromised as indicated in the outgrowth assay.

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子代活化素 a 对于小鼠植入前胚胎发育以及胚胎干细胞的衍生和多能性是不可或缺的†。
在这项工作中,我们旨在确定激活蛋白 A 在小鼠胚胎发生的关键事件中的作用,并区分源于子代的蛋白和母体生殖道分泌的蛋白的功能。为此,我们记录了Inhba基因敲除胚胎的发育过程和表型,并通过延时成像和检测系特异性标记物,将其与杂合子和野生型胚胎进行了比较。我们发现,子代活化素 A 缺乏不会影响胚胎发育到囊胚期的过程和速度。Inhba 基因敲除的胚胎会形成功能性的上胚层,其产生胚胎干细胞的能力就证明了这一点。我们的研究首次表明,胚胎衍生的胚胎干细胞的衍生、培养维持和多能性与外源性和内源性活化素 A 无关。然而,正如胚胎生长试验所显示的那样,缺乏活化素A的胚胎的植入能力可能会受到影响。
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4.30%
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