نتایج جستجو برای: pluripotency specific

تعداد نتایج: 1040520  

Journal: :Human reproduction update 2006
Stephanie A Pangas Aleksandar Rajkovic

Transcription factors in the germline play important roles in ovary formation and folliculogenesis, and control both oocyte development and somatic cell function. Factor in the germline (Figla) and newborn ovary homeobox gene (Nobox) represent a growing number of oocyte-specific transcription factors that regulate genes unique to oocytes. Studies on oocyte-specific transcription factors are imp...

Journal: :Cell systems 2015
Cameron Sokolik Yanxia Liu David Bauer Jade McPherson Michael Broeker Graham Heimberg Lei S Qi David A Sivak Matt Thomson

Stem cells occupy variable environments where they must distinguish stochastic fluctuations from developmental cues. Here, we use optogenetics to investigate how the pluripotency network in embryonic stem (ES) cells achieves a robust response to differentiation cues but not to gene expression fluctuations. We engineered ES cells in which we could quantitatively ontrol the endogenous mechanism o...

2012
S.P. Medvedev E.A. Pokushalov S.M. Zakian

Pluripotency is maintained by a complex system that includes the genetic and epigenetic levels. Recent studies have shown that the genetic level (transcription factors, signal pathways, and microRNAs) closely interacts with the enzymes and other specific proteins that participate in the formation of the chromatin structure. The interaction between the two systems results in the unique chromatin...

2016
Victoria L. Mascetti Roger A. Pedersen

Pluripotent stem cells are defined by their capacity to differentiate into all three tissue layers that comprise the body. Chimera formation, generated by stem cell transplantation to the embryo, is a stringent assessment of stem cell pluripotency. However, the ability of human pluripotent stem cells (hPSCs) to form embryonic chimeras remains in question. Here we show using a stage-matching app...

Journal: :Journal of cell science 2012
Tomonobu Sato Fumihiko Okumura Tadashi Ariga Shigetsugu Hatakeyama

The proto-oncogene product Myc is a master regulator of cell proliferation through its specific binding to the E-box motif in genomic DNA. It has been reported that Myc has an important role in the proliferation and maintenance of the pluripotency of embryonic stem (ES) cells and that the transcriptional activity of Myc is regulated by several post-translational modifications, including ubiquit...

Journal: :Cell 2008
Jacob Hanna Styliani Markoulaki Patrick Schorderet Bryce W. Carey Caroline Beard Marius Wernig Menno P. Creyghton Eveline J. Steine John P. Cassady Ruth Foreman Christopher J. Lengner Jessica A. Dausman Rudolf Jaenisch

Pluripotent cells can be derived from fibroblasts by ectopic expression of defined transcription factors. A fundamental unresolved question is whether terminally differentiated cells can be reprogrammed to pluripotency. We utilized transgenic and inducible expression of four transcription factors (Oct4, Sox2, Klf4, and c-Myc) to reprogram mouse B lymphocytes. These factors were sufficient to co...

2015
Kyungjin Boo Jinhyuk Bhin Yoon Jeon Joomyung Kim Hi-Jai R. Shin Jong-Eun Park Kyeongkyu Kim Chang Rok Kim Hyonchol Jang In-Hoo Kim V. Narry Kim Daehee Hwang Ho Lee Sung Hee Baek

The actions of transcription factors, chromatin modifiers and noncoding RNAs are crucial for the programming of cell states. Although the importance of various epigenetic machineries for controlling pluripotency of embryonic stem (ES) cells has been previously studied, how chromatin modifiers cooperate with specific transcription factors still remains largely elusive. Here, we find that Pontin ...

2016
Irene Cantone Hakan Bagci Dirk Dormann Gopuraja Dharmalingam Tatyana Nesterova Neil Brockdorff Claire Rougeulle Celine Vallot Edith Heard Ronan Chaligne Matthias Merkenschlager Amanda G Fisher

Erasure of epigenetic memory is required to convert somatic cells towards pluripotency. Reactivation of the inactive X chromosome (Xi) has been used to model epigenetic reprogramming in mouse, but human studies are hampered by Xi epigenetic instability and difficulties in tracking partially reprogrammed iPSCs. Here we use cell fusion to examine the earliest events in the reprogramming-induced X...

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