Chromatin remodeling plays a vital role in the regulation of genes, affecting how DNA access. Disorders in this process can also lead to cancer and other diseases. To better understand how chromatin remodeling projects, scientists at Children’s Children’s Hospital St. Jude used the Cryo-Electron Microscopy (Cryo-EM) to obtain subtle structural details of a human chromatin reconstrator in action. The researchers occupied 13 structures that together offer a comprehensive view of how the enzyme SNF2H enzyme works, providing information that is likely to be distributed to other such enzymes. The project was published today Cell research.
Chromatin includes parts of DNA wrapped around proteins called tissues to form collective nucleosomes. A chromatin remodeling mechanism called “nucleosoma slip” allows a nucleosomes to move to control gene control, but the way it works is not fully understood. To treat this gap, Mario Halic, PhD, a section of St. Judas, used Cryo-Em to capture the SNF2H chromatin removal enzyme in action.
Previous tasks that typically occupied snapshots of the reformer “frozen” in a state. Here we were able to visualize the constant movement of an enzyme of chromatin remodeling while moving the DNA to nucleosomes. ”
Mario Halic, Phd, St. Jude Department of Structural Biology
Teasing the thinnest details of remodeling
SNF2H is a key enzyme in the remodeling of nucleosoma, the split of which has been associated with developmental disorders. Like other chromatin remodelists, SNF2H uses energy from ATP hydrolysis to slide nucleosomes. Extensive studies have helped to understand the process by providing snapshots of SNF2H trapped in different situations. On the contrary, Halic and his team looked at SNF2H to interact with nucleosomes in the presence of ATP, thereby recording the enzyme in action.
Data analysis has led the researchers to obtain 13 different structures of the SNF2H-Nockosome complex at various intermediate points along the nucleosle slip process. Organizing them in five groups allowed the researchers to identify the enzyme steps and reveal the complete dynamic picture of the slip sliding.
Researchers measure the functional significance of the various interactions within the structure by introducing specific mutations and intersections – artificial restrictions that lock a protein in shape to test the importance of specific movements in protein function. This work allowed them to tease previously conflicting observations to draw up a comprehensive description of the way in which sliding nucleosome works and its impact on gene regulation.
“Nucleosomes carry all genetic information within the core of the eukaryotic cell. Chromatin rehabilitors help access the cells and transmit this information,” said co-authored author Deepshikha Malik, PhD. “The dissection of the mechanics of the action of the redevelopers in nucleosomes is important to understand how our genome is expressed.”
Authors and funding
The other co-author of the study is Ashish Deshmukh, St. Jude. The other author of the study is Silvija Bilokapic, St. Jude.
The study was supported by grants by the National Institutes of Health (1R01gM135599 and 1R01GM141694) and the US Lebanese Syrian Charities (ALSAC), the St. Jude.
Source:
Magazine report:
Malik, D., et al. (2025). Chromatin remodeling mechanisms by human SNF2 Atpase SNF2H. Cell research. Doi.org/10.1038/S41422-025-01103-W.
