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      X chromosome inactivation in human development

      1 , 2 , 3 , 3
      Development
      The Company of Biologists

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          Naive and primed pluripotent states.

          After maternal predetermination gives way to zygotic regulation, a ground state is established within the mammalian embryo. This tabula rasa for embryogenesis is present only transiently in the preimplantation epiblast. Here, we consider how unrestricted cells are first generated and then prepared for lineage commitment. We propose that two phases of pluripotency can be defined: naive and primed. This distinction extends to pluripotent stem cells derived from embryos or by molecular reprogramming ex vivo.
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            The Istanbul consensus workshop on embryo assessment: proceedings of an expert meeting.

            Many variations in oocyte and embryo grading make inter-laboratory comparisons extremely difficult. This paper reports the proceedings of an international consensus meeting on oocyte and embryo morphology assessment. Background presentations about current practice were given. The expert panel developed a set of consensus points to define the minimum criteria for oocyte and embryo morphology assessment. It is expected that the definition of common terminology and standardization of laboratory practice related to embryo morphology assessment will result in more effective comparisons of treatment outcomes. This document is intended to be referenced as a global consensus to allow standardized reporting of the minimum data set required for the accurate description of embryo development.
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              Directly reprogrammed fibroblasts show global epigenetic remodeling and widespread tissue contribution.

              Ectopic expression of the four transcription factors Oct4, Sox2, c-Myc, and Klf4 is sufficient to confer a pluripotent state upon the fibroblast genome, generating induced pluripotent stem (iPS) cells. It remains unknown if nuclear reprogramming induced by these four factors globally resets epigenetic differences between differentiated and pluripotent cells. Here, using novel selection approaches, we have generated iPS cells from fibroblasts to characterize their epigenetic state. Female iPS cells showed reactivation of a somatically silenced X chromosome and underwent random X inactivation upon differentiation. Genome-wide analysis of two key histone modifications indicated that iPS cells are highly similar to ES cells. Consistent with these observations, iPS cells gave rise to viable high-degree chimeras with contribution to the germline. These data show that transcription factor-induced reprogramming leads to the global reversion of the somatic epigenome into an ES-like state. Our results provide a paradigm for studying the epigenetic modifications that accompany nuclear reprogramming and suggest that abnormal epigenetic reprogramming does not pose a problem for the potential therapeutic applications of iPS cells.
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                Author and article information

                Journal
                Development
                Development
                The Company of Biologists
                0950-1991
                1477-9129
                January 03 2020
                January 01 2020
                January 03 2020
                January 01 2020
                : 147
                : 1
                : dev183095
                Affiliations
                [1 ]Université de Paris, UMR 1016, Institut Cochin, 75014 Paris, France
                [2 ]Service de Biologie de la Reproduction – CECOS, Paris Centre Hospital, APHP.centre, 75014 Paris, France
                [3 ]Université de Paris, Epigenetics and Cell Fate, CNRS, F-75013 Paris, France
                Article
                10.1242/dev.183095
                31900287
                e03987e2-1a23-4d6a-934e-d070c6c9a18d
                © 2020

                http://www.biologists.com/user-licence-1-1

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