1. Nucleosome conformation dictates the histone code.
- Author
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Marunde MR, Fuchs HA, Burg JM, Popova IK, Vaidya A, Hall NW, Weinzapfel EN, Meiners MJ, Watson R, Gillespie ZB, Taylor HF, Mukhsinova L, Onuoha UC, Howard SA, Novitzky K, McAnarney ET, Krajewski K, Cowles MW, Cheek MA, Sun ZW, Venters BJ, Keogh MC, and Musselman CA
- Subjects
- Histone Code, Chromatin, Protein Processing, Post-Translational, Peptides metabolism, Nucleosomes, Histones metabolism
- Abstract
Histone post-translational modifications (PTMs) play a critical role in chromatin regulation. It has been proposed that these PTMs form localized 'codes' that are read by specialized regions (reader domains) in chromatin-associated proteins (CAPs) to regulate downstream function. Substantial effort has been made to define [CAP: histone PTM] specificities, and thus decipher the histone code and guide epigenetic therapies. However, this has largely been done using the reductive approach of isolated reader domains and histone peptides, which cannot account for any higher-order factors. Here, we show that the [BPTF PHD finger and bromodomain: histone PTM] interaction is dependent on nucleosome context. The tandem reader selectively associates with nucleosomal H3K4me3 and H3K14ac or H3K18ac, a combinatorial engagement that despite being in cis is not predicted by peptides. This in vitro specificity of the BPTF tandem reader for PTM-defined nucleosomes is recapitulated in a cellular context. We propose that regulatable histone tail accessibility and its impact on the binding potential of reader domains necessitates we refine the 'histone code' concept and interrogate it at the nucleosome level., Competing Interests: MM, JB, IP, AV, NH, EW, MM, RW, ZG, HT, LM, UO, SH, KN, EM, KK, MC, MC, ZS, BV Affiliated with EpiCypher Inc; the author has no financial interests to declare, HF, CM No competing interests declared, MK A board member of EpiCypher Inc; the author has no financial interests to declare, (© 2024, Marunde, Fuchs et al.)
- Published
- 2024
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