RT Journal Article SR Electronic T1 A Dynamic Mode of Mitotic Bookmarking by Transcription Factors JF bioRxiv FD Cold Spring Harbor Laboratory SP 066464 DO 10.1101/066464 A1 Sheila S. Teves A1 Luye An A1 Anders S. Hansen A1 Liangqi Xie A1 Xavier Darzacq A1 Robert Tjian YR 2016 UL http://biorxiv.org/content/early/2016/08/01/066464.abstract AB During mitosis, transcription is shut off, chromatin condenses, and most transcription factors (TFs) are reported to be excluded from chromosomes. How do daughter cells re-establish the original transcription program? Recent discoveries that a select set of TFs remain bound on mitotic chromosomes suggest a potential mechanism for maintaining transcriptional programs through the cell cycle termed mitotic bookmarking. Here we report instead that many TFs remain associated with chromosomes, and that the exclusion previously described is largely a fixation artifact. In particular, most TFs we tested are significantly enriched on mitotic chromosomes. Studies with Sox2 reveal that this mitotic interaction is more dynamic than in interphase and requires both DNA binding and nuclear import. Furthermore, this dynamic mode results from lack of transcriptional activation rather than decreased accessibility of underlying DNA sequences in mitosis. The nature of the cross-linking artifact prompts careful re-examination of the role of TFs in mitotic bookmarking.HighlightsMany transcription factors bind to mitotic chromosomesSox2 mitotic interaction is dynamic and requires DNA binding and nuclear importDNA remains highly accessible in mitotic chromosomesFormaldehyde-based cross-linking leads to mis-localization of TFs