Literature DB >> 11839785

Transient pluripotent cell populations during primitive ectoderm formation: correlation of in vivo and in vitro pluripotent cell development.

T A Pelton1, S Sharma, T C Schulz, J Rathjen, P D Rathjen.   

Abstract

Formation and differentiation of a pluripotent cell population is central to mammalian development, and the isolation, identification and manipulation of human pluripotent cells is predicted to be of therapeutic use. Within the early mammalian embryo, two distinct populations of pluripotent cells have been described: the inner cell mass (ICM), which differentiates to form a second pluripotent cell populations, the primitive ectoderm. Indirect evidence suggests the existence of temporally distinct intermediate pluripotent cell populations as primitive ectoderm is formed. We coupled an in vitro model of primitive ectoderm formation (the transition of embryonic stem cells to early primitive ectoderm-like (EPL) cells) with ddPCR-based techniques to identify three novel genes, Psc1, CRTR-1 and PRCE, that were expressed differently during pluripotent cell progression. Detailed mapping of these genes with Oct4, Rex1 and Fgf5 on pregastrulation embryos provided the first molecular evidence for the existence of successive, temporally distinct pluripotent cell populations in the embryo between the ICM and primitive ectoderm. No evidence was found for spatial heterogeneity within the Oct4(+) pool. The transition between populations correlated with morphological or developmental alterations in pluripotent cells in vivo. Genes that are temporally expressed during pluripotent cell progression may provide an opportunity for molecular discrimination of pluripotent cells at different stages of maturation in vivo and an understanding of the cellular origins and properties of pluripotent cell lines isolated from diverse sources. Furthermore, the strong correlation of gene expression demonstrated between EPL cell formation in vitro and primitive ectoderm formation in vivo validates EPL cells as a model for primitive ectoderm, thereby providing a model system for the investigation of pluripotent differentiation and an opportunity for directed differentiation of pluripotent cells to therapeutically useful cell populations.

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Year:  2002        PMID: 11839785     DOI: 10.1242/jcs.115.2.329

Source DB:  PubMed          Journal:  J Cell Sci        ISSN: 0021-9533            Impact factor:   5.235


  63 in total

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2.  Tracking the progression of the human inner cell mass during embryonic stem cell derivation.

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4.  Retinoic acid orchestrates fibroblast growth factor signalling to drive embryonic stem cell differentiation.

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Journal:  Development       Date:  2010-03       Impact factor: 6.868

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6.  Sequential development of hematopoietic and cardiac mesoderm during embryonic stem cell differentiation.

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7.  High-throughput screen for genes predominantly expressed in the ICM of mouse blastocysts by whole mount in situ hybridization.

Authors:  Toshiyuki Yoshikawa; Yulan Piao; Jinhui Zhong; Ryo Matoba; Mark G Carter; Yuxia Wang; Ilya Goldberg; Minoru S H Ko
Journal:  Gene Expr Patterns       Date:  2005-12-01       Impact factor: 1.224

8.  Directed neural differentiation of human embryonic stem cells via an obligated primitive anterior stage.

Authors:  Matthew T Pankratz; Xue-Jun Li; Timothy M Lavaute; Elizabeth A Lyons; Xin Chen; Su-Chun Zhang
Journal:  Stem Cells       Date:  2007-03-01       Impact factor: 6.277

9.  DGCR8 is essential for microRNA biogenesis and silencing of embryonic stem cell self-renewal.

Authors:  Yangming Wang; Rostislav Medvid; Collin Melton; Rudolf Jaenisch; Robert Blelloch
Journal:  Nat Genet       Date:  2007-01-28       Impact factor: 38.330

10.  Genome-wide dynamics of replication timing revealed by in vitro models of mouse embryogenesis.

Authors:  Ichiro Hiratani; Tyrone Ryba; Mari Itoh; Joy Rathjen; Michael Kulik; Bernadett Papp; Eden Fussner; David P Bazett-Jones; Kathrin Plath; Stephen Dalton; Peter D Rathjen; David M Gilbert
Journal:  Genome Res       Date:  2009-12-01       Impact factor: 9.043

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