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Trypanosome histone variants H3.V and H4.V promote nucleosome plasticity in repressed chromatin

Molecular Therapy. 2026-02; 
Gauri Deák, Hayden Burdett, James A Watson, Marcus D Wilson Centre for Cell Biology, University of Edinburgh, Michael Swann Building, Kings Buildings, Mayfield Road, Edinburgh EH9 3JR, UK; Institute of Quantitative Biology, Biochemistry and Biotechnology, University of Edinburgh, Michael Swann Building, Kings Buildings, Mayfield Road
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Abstract

Histone variants define distinct chromatin states by modulating the biophysical properties of nucleosomes. Variants play a particularly important role in the parasitic protist Trypanosoma brucei, which has unusual chromatin and lacks a canonical repressive heterochromatin system. Instead, T. brucei utilizes specialized divergent histone variants H3.V and H4.V. However, the biochemical basis of their repressive functions is unknown. Here, we determined the structure of the H3.V-H4.V nucleosome core particle and biochemically characterized variant-containing nucleosomes and nucleosome arrays, probing their unique properties. We discovered that surprisingly for repressive-state nucleosomes, H3.V promotes pronounce... More

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