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. 2016 Apr 25;44(15):7144–7158. doi: 10.1093/nar/gkw323

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Published by Oxford University Press on behalf of Nucleic Acids Research 2016. This work is written by (a) US Government employee(s) and is in the public domain in the US.

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Figure 6. — Loss of HMGNs enhances the occupancy of unstable nucleosomes at TSS in both resting and activated B cells. (A and B) Loss of HMGNs does not affect the kinetics of MNase digestion of resting cells. (C and D) Loss of HMGNs enhances the occupancy of unstable (C) but not of stable (D) nucleosomes at the TSS of resting cells. (E and F) Loss of HMGNs does not affect the kinetics of MNase digestion of activated cells. (G and H) Loss of HMGNs enhances occupancy of unstable (G) but not of stable (H) nucleosome at the TSS of activated cells. Resting and activated B cells were digested with increasing concentration of MNase (0.01–2 U/ml). Mononucleosomes from limited (L) and extensive (E) digestions were isolated, their DNA sequenced and aligned to the TSS of top 3000 expressed genes. Arrow points to the ‘nucleosome free’ region near the TSS.