Mitochondrial membrane dynamics control the shape, number, and distribution of mitochondria and regulate energy production and cell health. In a screen for yeast mutants with increased levels of templated insertions (~10-1000âbp) in the nuclear genome, we identified mitochondrial fusion deficient mutants (mgm1Î, ugo1Î, fzo1Î). We found that fusion mutants activate the iron regulon, have decreased iron-sulfur clusters (ISCs), and increased DNA damage, suggesting a role of iron homeostasis in preventing insertions. Consistently, a secondary screen found mutants affecting iron-sulfur cluster production (yfh1Î, grx5Î), vacuolar iron storage (ccc1Î) or general iron homeostasis (aft1Î) to exhibit high insertion levels. Treatment with iron chelators or hydrogen peroxide also increased insertions. We propose that iron dysregulation leading to oxidative DNA damage and compromised DNA repair drives insertions. These studies suggest that severe iron imbalance, associated with many human diseases and pharmacological treatments, can trigger genome instability in the form of templated insertions.
Deficits in mitochondrial dynamics and iron balance result in templated insertions.
线粒体动力学和铁平衡的缺陷会导致模板插入
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作者:Fox Jordan, Yu Yang, Yu Yang, Thakre Pilendra, Fox Chloe, Li Qian, Wang Yunxia, Hughes Adam, Wang Xin, Chen Kaifu, Ira Grzegorz
| 期刊: | Nature Communications | 影响因子: | 15.700 |
| 时间: | 2025 | 起止号: | 2025 Jul 1; 16(1):5454 |
| doi: | 10.1038/s41467-025-60546-2 | 研究方向: | 其它 |
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