The cohesin complex mediates DNA-DNA interactions both between (sister chromatid cohesion) and within chromosomes (DNA looping). It has been suggested that intra-chromosome loops are generated by extrusion of DNAs through the lumen of cohesin's ring. Scc2 (Nipbl) stimulates cohesin's ABC-like ATPase and is essential for loading cohesin onto chromosomes. However, it is possible that the stimulation of cohesin's ATPase by Scc2 also has a post-loading function, for example driving loop extrusion. Using fluorescence recovery after photobleaching (FRAP) and single-molecule tracking in human cells, we show that Scc2 binds dynamically to chromatin, principally through an association with cohesin. Scc2's movement within chromatin is consistent with a 'stop-and-go' or 'hopping' motion. We suggest that a low diffusion coefficient, a low stoichiometry relative to cohesin, and a high affinity for chromosomal cohesin enables Scc2 to move rapidly from one chromosomal cohesin complex to another, performing a function distinct from loading.
Scc2/Nipbl hops between chromosomal cohesin rings after loading.
Scc2/Nipbl 在加载后于染色体黏连蛋白环之间跳跃
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作者:Rhodes James, Mazza Davide, Nasmyth Kim, Uphoff Stephan
| 期刊: | Elife | 影响因子: | 6.400 |
| 时间: | 2017 | 起止号: | 2017 Sep 15; 6:e30000 |
| doi: | 10.7554/eLife.30000 | 研究方向: | 免疫/内分泌 |
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