| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2039872 | Cell Reports | 2014 | 9 Pages |
•The BAF180 chromatin remodeling subunit contributes to cohesion in mammalian cells•The cohesion defect is specific to the centromere•Cancer-associated mutations of BAF180 lead to defects in cohesion•Loss of BAF180 leads to dynamic chromosome instability
SummaryBAF180, a subunit of the PBAF chromatin remodeling complex, is frequently mutated in cancer. Although PBAF regulates transcription, it remains unclear whether this is what drives tumorigenesis in cells lacking BAF180. Based on data from yeast, we hypothesized that BAF180 may prevent tumorigenesis by promoting cohesion. Here, we show BAF180 is required for centromeric cohesion in mouse and human cells. Mutations identified in tumor samples are unable to support this activity, and also compromise cohesion-dependent functions in yeast. We provide evidence of genome instability in line with loss of cohesion, and importantly, we find dynamic chromosome instability following DNA damage in cells lacking BAF180. These data demonstrate a function for BAF180 in promoting genome stability that is distinct from its well-characterized role in transcriptional regulation, uncovering a potent mechanism for its tumor-suppressor activity.
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