Condensin targets and reduces unwound DNA structures associated with transcription in mitotic chromosome condensation

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作者
Takashi Sutani
Toyonori Sakata
Ryuichiro Nakato
Koji Masuda
Mai Ishibashi
Daisuke Yamashita
Yutaka Suzuki
Tatsuya Hirano
Masashige Bando
Katsuhiko Shirahige
机构
[1] Research Center for Epigenetic Disease,Department of Medical Genome Sciences
[2] Institute of Molecular and Cellular Biosciences,undefined
[3] The University of Tokyo,undefined
[4] Chromosome Dynamics Laboratory,undefined
[5] RIKEN,undefined
[6] Graduate School of Frontier Sciences,undefined
[7] The University of Tokyo,undefined
[8] CREST,undefined
[9] Japan Science and Technology Agency (JST),undefined
[10] Present address: Otsuka Pharmaceutical Co.,undefined
[11] Ltd,undefined
[12] Ako,undefined
[13] Hyogo 678-0207,undefined
[14] Japan.,undefined
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Chromosome condensation is a hallmark of mitosis in eukaryotes and is a prerequisite for faithful segregation of genetic material to daughter cells. Here we show that condensin, which is essential for assembling condensed chromosomes, helps to preclude the detrimental effects of gene transcription on mitotic condensation. ChIP-seq profiling reveals that the fission yeast condensin preferentially binds to active protein-coding genes in a transcription-dependent manner during mitosis. Pharmacological and genetic attenuation of transcription largely rescue bulk chromosome segregation defects observed in condensin mutants. We also demonstrate that condensin is associated with and reduces unwound DNA segments generated by transcription, providing a direct link between an in vitro activity of condensin and its in vivo function. The human condensin isoform condensin I also binds to unwound DNA regions at the transcription start sites of active genes, implying that our findings uncover a fundamental feature of condensin complexes.
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