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子宫内早期灵长类动物原肠胚形成的空间分析。

Spatial profiling of early primate gastrulation in utero.

机构信息

Department of Physiology, Development and Neuroscience, University of Cambridge, Cambridge, UK.

Centre for Trophoblast Research, University of Cambridge, Cambridge, UK.

出版信息

Nature. 2022 Sep;609(7925):136-143. doi: 10.1038/s41586-022-04953-1. Epub 2022 Jun 16.

Abstract

Gastrulation controls the emergence of cellular diversity and axis patterning in the early embryo. In mammals, this transformation is orchestrated by dynamic signalling centres at the interface of embryonic and extraembryonic tissues. Elucidating the molecular framework of axis formation in vivo is fundamental for our understanding of human development and to advance stem-cell-based regenerative approaches. Here we illuminate early gastrulation of marmoset embryos in utero using spatial transcriptomics and stem-cell-based embryo models. Gaussian process regression-based 3D transcriptomes delineate the emergence of the anterior visceral endoderm, which is hallmarked by conserved (HHEX, LEFTY2, LHX1) and primate-specific (POSTN, SDC4, FZD5) factors. WNT signalling spatially coordinates the formation of the primitive streak in the embryonic disc and is counteracted by SFRP1 and SFRP2 to sustain pluripotency in the anterior domain. Amnion specification occurs at the boundaries of the embryonic disc through ID1, ID2 and ID3 in response to BMP signalling, providing a developmental rationale for amnion differentiation of primate pluripotent stem cells (PSCs). Spatial identity mapping demonstrates that primed marmoset PSCs exhibit the highest similarity to the anterior embryonic disc, whereas naive PSCs resemble the preimplantation epiblast. Our 3D transcriptome models reveal the molecular code of lineage specification in the primate embryo and provide an in vivo reference to decipher human development.

摘要

原肠胚形成控制着早期胚胎中细胞多样性和轴模式的出现。在哺乳动物中,这种转变是由胚胎和胚胎外组织界面处的动态信号中心协调的。阐明体内轴形成的分子框架对于我们理解人类发育和推进基于干细胞的再生方法至关重要。在这里,我们使用空间转录组学和基于干细胞的胚胎模型来阐明狨猴胚胎的早期原肠胚形成。基于高斯过程回归的 3D 转录组描绘了前内脏内胚层的出现,其特征是保守的(HHEX、LEFTY2、LHX1)和灵长类特异性的(POSTN、SDC4、FZD5)因子。WNT 信号在胚胎盘中空间协调原始条纹的形成,并通过 SFRP1 和 SFRP2 来拮抗,以维持前域的多能性。羊膜的特化是通过 ID1、ID2 和 ID3 对 BMP 信号的反应在胚胎盘的边界处发生的,为灵长类多能干细胞(PSCs)的羊膜分化提供了发育学依据。空间身份映射表明,启动的狨猴 PSCs 与前胚胎盘具有最高的相似性,而原始 PSCs 则类似于植入前的上胚层。我们的 3D 转录组模型揭示了灵长类胚胎中谱系特化的分子密码,并提供了一个体内参考,以破译人类发育。

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