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Chemically Synthesized H3K14Ub Unveils Clr4's IDR-Mediated Multivalent Nucleosome Recognition in H3K9 Methylation

ANGEWANDTE CHEMIE International Edition. 2026-03; 
Maoshen Sun, Yunxiang Du, Zhengqing Li, Akejiang Aderjiang, Meixuan Xin, Huasong Ai
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Abstract

Histone H3 lysine 9 methylation (H3K9me) is a central epigenetic mark governing heterochromatin formation. Although the H3K9 methyltransferase Clr4 has been extensively characterized using short histone peptide substrates, how it recognizes and coordinates different structural domains to engage physiological substrate nucleosomes remains poorly understood. Here, we employed chemical protein synthesis to generate site-specifically ubiquitinated H3K14Ub histones and nucleosomes, enabling quantitative biochemical and structural investigations. Using a CAET handle-assisted strategy, we obtained homogeneous H3K14Ub nucleosomes and demonstrated that ubiquitination enhances Clr4 activity by ∼350-fold on nucleosomes ... More

Keywords

chemical protein synthesis; histone modification; quantitative activity reconstruction; site‐directed photo‐crosslinking strategy.