Controlled modelling of human epiblast and amnion development using stem cells

被引:0
|
作者
Yi Zheng
Xufeng Xue
Yue Shao
Sicong Wang
Sajedeh Nasr Esfahani
Zida Li
Jonathon M. Muncie
Johnathon N. Lakins
Valerie M. Weaver
Deborah L. Gumucio
Jianping Fu
机构
[1] University of Michigan,Department of Mechanical Engineering
[2] University of California,Department of Surgery, Center for Bioengineering and Tissue Regeneration
[3] San Francisco,Graduate Program in Bioengineering
[4] University of California,Department of Bioengineering and Therapeutic Sciences, Eli and Edythe Broad Center of Regeneration Medicine and Stem Cell Research
[5] San Francisco and University of California,Department of Radiation Oncology, Helen Diller Family Comprehensive Cancer Center
[6] Berkeley,Department of Cell and Developmental Biology
[7] University of California,Department of Biomedical Engineering
[8] San Francisco,undefined
[9] University of California,undefined
[10] San Francisco,undefined
[11] University of Michigan Medical School,undefined
[12] University of Michigan,undefined
来源
Nature | 2019年 / 573卷
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学科分类号
摘要
Early human embryonic development involves extensive lineage diversification, cell-fate specification and tissue patterning1. Despite its basic and clinical importance, early human embryonic development remains relatively unexplained owing to interspecies divergence2,3 and limited accessibility to human embryo samples. Here we report that human pluripotent stem cells (hPSCs) in a microfluidic device recapitulate, in a highly controllable and scalable fashion, landmarks of the development of the epiblast and amniotic ectoderm parts of the conceptus, including lumenogenesis of the epiblast and the resultant pro-amniotic cavity, formation of a bipolar embryonic sac, and specification of primordial germ cells and primitive streak cells. We further show that amniotic ectoderm-like cells function as a signalling centre to trigger the onset of gastrulation-like events in hPSCs. Given its controllability and scalability, the microfluidic model provides a powerful experimental system to advance knowledge of human embryology and reproduction. This model could assist in the rational design of differentiation protocols of hPSCs for disease modelling and cell therapy, and in high-throughput drug and toxicity screens to prevent pregnancy failure and birth defects.
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页码:421 / 425
页数:4
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