THE BRM-HDAC3-ERM REPRESSOR COMPLEX SUPPRESSES DEDIFFERENTIATION IN DROSOPHILA TYPE II NEUROBLAST LINEAGES

The Brm-HDAC3-Erm repressor complex suppresses dedifferentiation in Drosophila type II neuroblast lineages

The Brm-HDAC3-Erm repressor complex suppresses dedifferentiation in Drosophila type II neuroblast lineages

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The control of self-renewal click here and differentiation of neural stem and progenitor cells is a crucial issue in stem cell and cancer biology.Drosophila type II neuroblast lineages are prone to developing impaired neuroblast homeostasis if the limited self-renewing potential of intermediate neural progenitors (INPs) is unrestrained.Here, we demonstrate that Drosophila SWI/SNF chromatin remodeling Brahma (Brm) complex functions cooperatively with another chromatin remodeling factor, Histone deacetylase 3 (HDAC3) to suppress the formation of ectopic type II neuroblasts.

We show that multiple components of the animed aniflex complete Brm complex and HDAC3 physically associate with Earmuff (Erm), a type II-specific transcription factor that prevents dedifferentiation of INPs into neuroblasts.Consistently, the predicted Erm-binding motif is present in most of known binding loci of Brm.Furthermore, brm and hdac3 genetically interact with erm to prevent type II neuroblast overgrowth.

Thus, the Brm-HDAC3-Erm repressor complex suppresses dedifferentiation of INPs back into type II neuroblasts.

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