Recognition of shorter and longer trimethyllysine analogues by epigenetic reader proteins.

Histone Nε -lysine methylation is a widespread posttranslational modification that is specifically recognised by a diverse class of Nε -methyllysine binding reader proteins. Combined thermodynamic data, molecular dynamics simulations, and quantum chemical studies reveal that reader proteins efficiently bind trimethylornithine and trimethylhomolysine, the simplest Nε -trimethyllysine analogues that differ in the length of the side chain.