Delineation of the Protein Module That Anchors HMGN Proteins to Nucleosomes in the Chromatin of Living Cells
Delineation of the Protein Module That Anchors HMGN Proteins to Nucleosomes in the Chromatin of Living Cells
Numerous nuclear proteins bind to chromatin by targeting unique DNA sequences or specific histone modifications. In contrast, HMGN proteins recognize the generic structure of the 147-bp nucleosome core particle. HMGNs alter the structure and activity of chromatin by binding to nucleosomes; however, the determinants of the specific interaction of HMGNs with chromatin are not known. Here we use systematic mutagenesis, quantitative fluorescence recovery after photobleaching, fluorescence imaging, and mobility shift assays to identify the determinants important for the specific binding of these proteins to both the chromatin of living cells and to purified nucleosomes. We find that several regions of the protein affect the affinity of HMGNs to chromatin; however, the conserved sequence RRSARLSA, is the sole determinant of the specific interaction of HMGNs with nucleosomes. Within this sequence, each of the 4 amino acids in the R-S-RL motif are the only residues absolutely essential for anchoring HMGN protein to nucleosomes, both in vivo and in vitro. Our studies identify a new chromatin-binding module that specifically recognizes nucleosome cores independently of DNA sequence or histone tail modifications.
- University of Lyon System France
- National Institute of Health Pakistan
- Délégation Ile-de-France Sud France
- French National Centre for Scientific Research France
- Claude Bernard University Lyon 1 France
Mice, Knockout, HMGN2 Protein, Amino Acid Motifs, Molecular Sequence Data, Chromatin, Nucleosomes, Mice, Mutation, Animals, Amino Acid Sequence, Cells, Cultured, HMGN1 Protein, Protein Binding
Mice, Knockout, HMGN2 Protein, Amino Acid Motifs, Molecular Sequence Data, Chromatin, Nucleosomes, Mice, Mutation, Animals, Amino Acid Sequence, Cells, Cultured, HMGN1 Protein, Protein Binding
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