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Molecular Basis for Cohesin Acetylation by Establishment of Sister Chromatid Cohesion N-Acetyltransferase ESCO1.

J. Biol. Chem.. 2016; 
Rivera-Colón Yadilette,Maguire Andrew,Liszczak Glen P,Olia Adam S,Marmorstein R
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Peptide Synthesis For kcat and KM determination for peptide, near saturating concentrations of Ac- CoA (1 mM) was used in all enzymatic reactions, and the substrate peptide (NH2- SLRRVIGAKKDQYFLDKKMVT-COOH; GenScript) concentration was varied from 10 to 1,000 µM. Get A Quote

摘要

Protein acetylation is a prevalent posttranslational modification that is regulated by diverse acetyltransferase enzymes. Although histone acetyltransferases (HATs) have been well characterized both structurally and mechanistically, far less is known about non-histone acetyltransferase enzymes. The human ESCO1 and ESCO2 paralogs acetylate the cohesin complex subunit SMC3 to regulate the separation of sister chromatids during mitosis and meiosis. Missense mutations within the acetyltransferase domain of these proteins correlate with diseases, including endometrial cancers and Roberts syndrome. Despite their biological importance, the mechanisms underlying acetylation by the ESCO proteins are not understood... More

关键词

ESCO1,SMC3,X-ray crystallography,acetyltransferase,cell division,chromatin regulation,cohesin,crystal structure,enzyme structure,gene expression,posttranslational modification (PTM),protein acylation,protein structure,structure-func