The class I-specific HDAC inhibitor MS-275 modulates the differentiation potential of mouse embryonic stem cells

نویسندگان

  • Gianluigi Franci
  • Laura Casalino
  • Francesca Petraglia
  • Marco Miceli
  • Roberta Menafra
  • Branka Radic
  • Valeria Tarallo
  • Monica Vitale
  • Marzia Scarfò
  • Gabriella Pocsfalvi
  • Alfonso Baldi
  • Concetta Ambrosino
  • Nicola Zambrano
  • Eduardo Patriarca
  • Sandro De Falco
  • Gabriella Minchiotti
  • Hendrik G. Stunnenberg
  • Lucia Altucci
چکیده

Exploitation of embryonic stem cells (ESC) for therapeutic use and biomedical applications is severely hampered by the risk of teratocarcinoma formation. Here, we performed a screen of selected epi-modulating compounds and demonstrate that a transient exposure of mouse ESC to MS-275 (Entinostat), a class I histone deacetylase inhibitor (HDAC), modulates differentiation and prevents teratocarcinoma formation. Morphological and molecular data indicate that MS-275-primed ESCs are committed towards neural differentiation, which is supported by transcriptome analyses. Interestingly, in vitro withdrawal of MS-275 reverses the primed cells to the pluripotent state. In vivo, MS275-primed ES cells injected into recipient mice give only rise to benign teratomas but not teratocarcinomas with prevalence of neural-derived structures. In agreement, MS-275-primed ESC are unable to colonize blastocysts. These findings provide evidence that a transient alteration of acetylation alters the ESC fate.

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عنوان ژورنال:

دوره 2  شماره 

صفحات  -

تاریخ انتشار 2013