Litcius/Paper detail

Chromatin Reorganization during Myoblast Differentiation Involves the Caspase-Dependent Removal of SATB2

Ryan A. V. Bell, Mohammad Al‐Khalaf, Steve Brunette, Dalal Alsowaida, Alphonse Chu, Hina Bandukwala, Georg Dechant, Galina Apostolova, F. Jeffrey Dilworth, Lynn A. Megeney

2022Cells18 citationsDOIOpen Access PDF

Abstract

The induction of lineage-specific gene programs are strongly influenced by alterations in local chromatin architecture. However, key players that impact this genome reorganization remain largely unknown. Here, we report that the removal of the special AT-rich binding protein 2 (SATB2), a nuclear protein known to bind matrix attachment regions, is a key event in initiating myogenic differentiation. The deletion of myoblast SATB2 in vitro initiates chromatin remodeling and accelerates differentiation, which is dependent on the caspase 7-mediated cleavage of SATB2. A genome-wide analysis indicates that SATB2 binding within chromatin loops and near anchor points influences both loop and sub-TAD domain formation. Consequently, the chromatin changes that occur with the removal of SATB2 lead to the derepression of differentiation-inducing factors while also limiting the expression of genes that inhibit this cell fate change. Taken together, this study demonstrates that the temporal control of the SATB2 protein is critical in shaping the chromatin environment and coordinating the myogenic differentiation program.

Topics & Concepts

ChromatinCell biologyChromatin remodelingScaffold/matrix attachment regionDerepressionBiologyCellular differentiationGeneGeneticsGene expressionPsychological repressionGenomics and Chromatin DynamicsRNA Research and SplicingCancer-related gene regulation
Chromatin Reorganization during Myoblast Differentiation Involves the Caspase-Dependent Removal of SATB2 | Litcius