1. Chromosomes and Gene Expression
  2. Genetics and Genomics

MOF-associated complexes ensure stem cell identity and Xist repression

  1. Tomasz Chelmicki
  2. Friederike Dündar
  3. Matthew Turley
  4. Tasneem Khanam
  5. Tugce Aktas
  6. Fidel Ramírez
  7. Anne-Valerie Gendrel
  8. Patrick R Wright
  9. Pavankumar Videm
  10. Rolf Backofen
  11. Edith Heard
  12. Thomas Manke
  13. Asifa Akhtar  Is a corresponding author
  1. Max Planck Institute for Immunobiology and Epigenetics, Germany
  2. Institute Curie, France
  3. University of Freiburg, Germany
  4. Institut Curie, France
https://doi.org/10.7554/eLife.02024
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  1. Tomasz Chelmicki
  2. Friederike Dündar
  3. Matthew Turley
  4. Tasneem Khanam
  5. Tugce Aktas
  6. Fidel Ramírez
  7. Anne-Valerie Gendrel
  8. Patrick R Wright
  9. Pavankumar Videm
  10. Rolf Backofen
  11. Edith Heard
  12. Thomas Manke
  13. Asifa Akhtar
(2014)
MOF-associated complexes ensure stem cell identity and Xist repression
eLife 3:e02024.
https://doi.org/10.7554/eLife.02024
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Abstract

Histone acetyl transferases (HATs) play distinct roles in many cellular processes and are frequently misregulated in cancers. Here, we study the regulatory potential of MYST1-(MOF)-containing MSL and NSL complexes in mouse embryonic stem cells (ESCs) and neuronal progenitors. We find that both complexes influence transcription by targeting promoters as well as TSS-distal enhancers. In contrast to flies, the MSL complex is not exclusively enriched on the X chromosome yet it is crucial for mammalian X chromosome regulation as it specifically regulates Tsix, the major repressor of Xist lncRNA. MSL depletion leads to decreased Tsix expression, reduced REX1 recruitment, and consequently, enhanced accumulation of Xist and variable numbers of inactivated X chromosomes during early differentiation. The NSL complex provides additional, Tsix-independent repression of Xist by maintaining pluripotency. MSL and NSL complexes therefore act synergistically by using distinct pathways to ensure a fail-safe mechanism for the repression of X inactivation in ESCs.

Article and author information

Author details

  1. Tomasz Chelmicki

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  2. Friederike Dündar

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  3. Matthew Turley

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  4. Tasneem Khanam

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  5. Tugce Aktas

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  6. Fidel Ramírez

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  7. Anne-Valerie Gendrel

    Institute Curie, Paris, France
    Competing interests
    No competing interests declared.

  8. Patrick R Wright

    University of Freiburg, Freiburg, Germany
    Competing interests
    No competing interests declared.

  9. Pavankumar Videm

    University of Freiburg, Freiburg, Germany
    Competing interests
    No competing interests declared.

  10. Rolf Backofen

    University of Freiburg, Freiburg, Germany
    Competing interests
    No competing interests declared.

  11. Edith Heard

    Institut Curie, Paris, France
    Competing interests
    No competing interests declared.

  12. Thomas Manke

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    Competing interests
    No competing interests declared.

  13. Asifa Akhtar

    Max Planck Institute for Immunobiology and Epigenetics, Freiburg, Germany
    For correspondence
    akhtar@immunbio.mpg.de
    Competing interests
    Asifa Akhtar, Reviewing editor, eLife.

Reviewing Editor

  1. Danny Reinberg, Howard Hughes Medical Institute, New York University School of Medicine, United States

Version history

  1. Received: December 6, 2013
  2. Accepted: May 11, 2014
  3. Accepted Manuscript published: May 19, 2014 (version 1)
  4. Version of Record published: June 17, 2014 (version 2)

Copyright

© 2014, Chelmicki et al.

This article is distributed under the terms of the Creative Commons Attribution License permitting unrestricted use and redistribution provided that the original author and source are credited.

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  1. Tomasz Chelmicki
  2. Friederike Dündar
  3. Matthew Turley
  4. Tasneem Khanam
  5. Tugce Aktas
  6. Fidel Ramírez
  7. Anne-Valerie Gendrel
  8. Patrick R Wright
  9. Pavankumar Videm
  10. Rolf Backofen
  11. Edith Heard
  12. Thomas Manke
  13. Asifa Akhtar
(2014)
MOF-associated complexes ensure stem cell identity and Xist repression
eLife 3:e02024.
https://doi.org/10.7554/eLife.02024

Share this article

https://doi.org/10.7554/eLife.02024

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    Mof-associated complexes have overlapping and unique roles in regulating pluripotency in embryonic stem cells and during differentiation

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