Cockayne syndrome group B deficiency reduces H3K9me3 chromatin remodeler SETDB1 and exacerbates cellular aging

Jong-Hyuk Lee, Tyler G. Demarest, Mansi Babbar, Edward W. Kim, Mustafa N. Okur, Supriyo De, Deborah L. Croteau, Vilhelm A. Bohr

Research output: Contribution to journalJournal articleResearchpeer-review

26 Citations (Scopus)

Abstract

Cockayne syndrome is an accelerated aging disorder, caused by mutations in the CSA or CSB genes. In CSB-deficient cells, poly (ADP ribose) polymerase (PARP) is persistently activated by unrepaired DNA damage and consumes and depletes cellular nicotinamide adenine dinucleotide, which leads to mitochondrial dysfunction. Here, the distribution of poly (ADP ribose) (PAR) was determined in CSB-deficient cells using ADPr-ChAP (ADP ribose-chromatin affinity purification), and the results show striking enrichment of PAR at transcription start sites, depletion of heterochromatin and downregulation of H3K9me3-specific methyltransferases SUV39H1 and SETDB1. Induced-expression of SETDB1 in CSB-deficient cells downregulated PAR and normalized mitochondrial function. The results suggest that defects in CSB are strongly associated with loss of heterochromatin, downregulation of SETDB1, increased PAR in highly-transcribed regions, and mitochondrial dysfunction.
Original languageEnglish
JournalNucleic Acids Research
Volume47
Issue number16
Pages (from-to)8548-8562
ISSN0305-1048
DOIs
Publication statusPublished - 2019

Cite this