熊本大学のノウハウを活かした新たなカタチの大学院教育

英語
日本
セミナー・シンポジウム及び募集
Seminar & Symposium/Admissions
2017-07-19

最先端研究セミナー

 

講演者: 関 由行 (関西学院大学 理工学部 生命科学科 関研究室 准教授)

演題: Evolutionary and functional analysis of PRDM14 in pluripotent cells and primordial germ cells

 

日時: 7月19日(水) 12:00-13:00

会場: 発生医学研究所1階 カンファレンス室

 

Abstract:

Germ cell specification in multicellular organisms is subdivided to two modes: “preformation” and “epigenesis”. In epigenesis, fertilized egg firstly establishes pluripotent cell, which can give rise to both germ and somatic cells, and germ cells are induced from pluripotent cells by receiving the inducing signals. The molecular network ensuring the pluripotency is controlled by core circuitry of transcription factors including POU5F1, SOX2 and Nanog. We have previously shown that PR-domain containing 14 (PRDM14) stabilized core circuitry of pluripotent factors in the maintenance and induction of pluripotency mediated by active DNA demethylation.

In this talk, I’d like to present recent work regarding the functional and gene expression comparison of PRDM14 orthologs in deuterostomes. Amphioxus (Cephalochordate) and Zebrafish (Teleost) but not Sea urchin (Echinodermata) PRDM14 could rescue mouse PRDM14 functions in the maintenance of ESC pluripotency. The expression of Prdm14 is restricted to pluripotent cells and primordial germ cells in mammals, however, Prdm14 was expressed in motor neuron but not in germ cells in amphioxus embryo as observed in zebrafish. Our data suggest that evolutionary changes of cis-regulatory elements surrounding at Prdm14 gene might integrate PRDM14 into pluripotent network of transcription factors.

 

 

References

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  3. Ohno, R., Nakayama, M., Naruse., Okashita, N., Takano, O., Tachibana, M., Asano, M., Saitou, M. and Seki, Y., Development, 2013
  4. #Yamaji, M., #Seki, Y., #Kurimoto, K., Yabuta, Y., Yuasa, M., Shigeta, M., Yamanaka., K., Ohinata., Y., and Saitou, M., Nature Genetics, 2008

 

担当分野: 組織幹細胞分野 小川(内線:6591)

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