Snf2h-mediated chromatin organization and histone H1 dynamics govern cerebellar morphogenesis and neural maturation

Snf2h 介导的染色质组织和组蛋白 H1 动力学控制小脑形态发生和神经成熟

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作者:Matías Alvarez-Saavedra, Yves De Repentigny, Pamela S Lagali, Edupuganti V S Raghu Ram, Keqin Yan, Emile Hashem, Danton Ivanochko, Michael S Huh, Doo Yang, Alan J Mears, Matthew A M Todd, Chelsea P Corcoran, Erin A Bassett, Nicholas J A Tokarew, Juraj Kokavec, Romit Majumder, Ilya Ioshikhes, Valerie

Abstract

Chromatin compaction mediates progenitor to post-mitotic cell transitions and modulates gene expression programs, yet the mechanisms are poorly defined. Snf2h and Snf2l are ATP-dependent chromatin remodelling proteins that assemble, reposition and space nucleosomes, and are robustly expressed in the brain. Here we show that mice conditionally inactivated for Snf2h in neural progenitors have reduced levels of histone H1 and H2A variants that compromise chromatin fluidity and transcriptional programs within the developing cerebellum. Disorganized chromatin limits Purkinje and granule neuron progenitor expansion, resulting in abnormal post-natal foliation, while deregulated transcriptional programs contribute to altered neural maturation, motor dysfunction and death. However, mice survive to young adulthood, in part from Snf2l compensation that restores Engrailed-1 expression. Similarly, Purkinje-specific Snf2h ablation affects chromatin ultrastructure and dendritic arborization, but alters cognitive skills rather than motor control. Our studies reveal that Snf2h controls chromatin organization and histone H1 dynamics for the establishment of gene expression programs underlying cerebellar morphogenesis and neural maturation.

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