Affiliation:
1. Department of Biomedical Engineering University of Michigan Ann Arbor Michigan USA
2. Biointerfaces Institute University of Michigan Ann Arbor Michigan USA
3. Program in Cellular and Molecular Biology University of Michigan Ann Arbor Michigan USA
4. Department of Computational Medicine & Bioinformatics University of Michigan Ann Arbor Michigan USA
5. Department of Human Genetics University of Michigan Ann Arbor Michigan USA
Abstract
AbstractAge‐related skeletal muscle atrophy or sarcopenia is a significant societal problem that is becoming amplified as the world's population continues to increase. The regeneration of damaged skeletal muscle is mediated by muscle stem cells, but in old age muscle stem cells become functionally attenuated. The molecular mechanisms that govern muscle stem cell aging encompass changes across multiple regulatory layers and are integrated by the three‐dimensional organization of the genome. To quantitatively understand how hierarchical chromatin architecture changes during muscle stem cell aging, we generated 3D chromatin conformation maps (Hi‐C) and integrated these datasets with multi‐omic (chromatin accessibility and transcriptome) profiles from bulk populations and single cells. We observed that muscle stem cells display static behavior at global scales of chromatin organization during aging and extensive rewiring of local contacts at finer scales that were associated with variations in transcription factor binding and aberrant gene expression. These data provide insights into genome topology as a regulator of molecular function in stem cell aging.
Funder
3M Foundation
American Federation for Aging Research
Congressionally Directed Medical Research Programs
Defense Advanced Research Projects Agency
National Institute of Arthritis and Musculoskeletal and Skin Diseases
National Institute of Biomedical Imaging and Bioengineering
National Institute on Aging
National Science Foundation of Sri Lanka
Cited by
8 articles.
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