Balanced SET levels favor the correct enhancer repertoire during cell fate acquisition

Author:

Zaghi Mattia,Banfi Federica,Massimino Luca,Volpin MonicaORCID,Bellini EdoardoORCID,Brusco Simone,Merelli Ivan,Barone Cristiana,Bruni Michela,Bossini Linda,Lamparelli Luigi Antonio,Pintado Laura,D’Aliberti Deborah,Spinelli Silvia,Mologni LucaORCID,Colasante GaiaORCID,Ungaro Federica,Cioni Jean-Michel,Azzoni EmanueleORCID,Piazza RoccoORCID,Montini EugenioORCID,Broccoli VaniaORCID,Sessa AlessandroORCID

Abstract

AbstractWithin the chromatin, distal elements interact with promoters to regulate specific transcriptional programs. Histone acetylation, interfering with the net charges of the nucleosomes, is a key player in this regulation. Here, we report that the oncoprotein SET is a critical determinant for the levels of histone acetylation within enhancers. We disclose that a condition in which SET is accumulated, the severe Schinzel-Giedion Syndrome (SGS), is characterized by a failure in the usage of the distal regulatory regions typically employed during fate commitment. This is accompanied by the usage of alternative enhancers leading to a massive rewiring of the distal control of the gene transcription. This represents a (mal)adaptive mechanism that, on one side, allows to achieve a certain degree of differentiation, while on the other affects the fine and corrected maturation of the cells. Thus, we propose the differential in cis-regulation as a contributing factor to the pathological basis of SGS and possibly other the SET-related disorders in humans.

Funder

Ministero della Salute

Career Development Award from the Giovanni Armenise-Harvard Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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