Genome-wide analysis of EGR2/SOX10 binding in myelinating peripheral nerve

R Srinivasan, G Sun, S Keles, EA Jones… - Nucleic acids …, 2012 - academic.oup.com
R Srinivasan, G Sun, S Keles, EA Jones, SW Jang, C Krueger, JJ Moran, J Svaren
Nucleic acids research, 2012academic.oup.com
Myelin is essential for the rapidity of saltatory nerve conduction, and also provides trophic
support for axons to prevent axonal degeneration. Two critical determinants of myelination
are SOX10 and EGR2/KROX20. SOX10 is required for specification of Schwann cells from
neural crest, and is required at every stage of Schwann cell development. Egr2/Krox20
expression is activated by axonal signals in myelinating Schwann cells, and is required for
cell cycle arrest and myelin formation. To elucidate the integrated function of these two …
Abstract
Myelin is essential for the rapidity of saltatory nerve conduction, and also provides trophic support for axons to prevent axonal degeneration. Two critical determinants of myelination are SOX10 and EGR2/KROX20. SOX10 is required for specification of Schwann cells from neural crest, and is required at every stage of Schwann cell development. Egr2/Krox20 expression is activated by axonal signals in myelinating Schwann cells, and is required for cell cycle arrest and myelin formation. To elucidate the integrated function of these two transcription factors during peripheral nerve myelination, we performed in vivo ChIP-Seq analysis of myelinating peripheral nerve. Integration of these binding data with loss-of-function array data identified a range of genes regulated by these factors. In addition, although SOX10 itself regulates Egr2/Krox20 expression, leading to coordinate activation of several major myelin genes by the two factors, there is a large subset of genes that are activated independent of EGR2. Finally, the results identify a set of SOX10-dependent genes that are expressed in early Schwann cell development, but become subsequently repressed by EGR2/KROX20.
Oxford University Press