h3k9me23 binding of the mbt domain protein lin-61 is essential for caenorhabditis elegans vulva development林h3k9me23绑定mbt域的蛋白- 61对秀丽隐杆线虫阴户发展至关重要.pdfVIP
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h3k9me23 binding of the mbt domain protein lin-61 is essential for caenorhabditis elegans vulva development林h3k9me23绑定mbt域的蛋白- 61对秀丽隐杆线虫阴户发展至关重要
H3K9me2/3 Binding of the MBT Domain Protein LIN-61 Is
Essential for Caenorhabditis elegans Vulva Development
Nora Koester-Eiserfunke, Wolfgang Fischle*
¨
Laboratory of Chromatin Biochemistry, Max Planck Institute for Biophysical Chemistry, Gottingen, Germany
Abstract
MBT domain proteins are involved in developmental processes and tumorigenesis. In vitro binding and mutagenesis studies
have shown that individual MBT domains within clustered MBT repeat regions bind mono- and dimethylated histone lysine
residues with little to no sequence specificity but discriminate against the tri- and unmethylated states. However, the exact
function of promiscuous histone methyl-lysine binding in the biology of MBT domain proteins has not been elucidated.
Here, we show that the Caenorhabditis elegans four MBT domain protein LIN-61, in contrast to other MBT repeat factors,
specifically interacts with histone H3 when methylated on lysine 9, displaying a strong preference for di- and trimethylated
states (H3K9me2/3). Although the fourth MBT repeat is implicated in this interaction, H3K9me2/3 binding minimally
requires MBT repeats two to four. Further, mutagenesis of residues conserved with other methyl-lysine binding MBT regions
in the fourth MBT repeat does not abolish interaction, implicating a distinct binding mode. In vivo, H3K9me2/3 interaction of
LIN-61 is required for C. elegans vulva development within the synMuvB pathway. Mutant LIN-61 proteins deficient in
H3K9me2/3 binding fail to rescue lin-61 synMuvB function. Also, previously identified point mutant synMuvB alleles are
deficient in H3K9me2/3 interaction although these target residues that are outside of the fourth MBT repeat. Interestingly,
lin-61 genetically interacts with two other synMuvB genes, hpl-2,
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