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Sumoylation Influences DNA Break Repair Partly by Increasing the Solubility of a Conserved End Resection Protein
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نویسنده
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sarangi p. ,steinacher r. ,altmannova v. ,fu q. ,paull t.t. ,krejci l. ,whitby m.c. ,zhao x.
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منبع
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plos genetics - 2015 - دوره : 11 - شماره : 1
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چکیده
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Protein modifications regulate both dna repair levels and pathway choice. how each modification achieves regulatory effects and how different modifications collaborate with each other are important questions to be answered. here,we show that sumoylation regulates double-strand break repair partly by modifying the end resection factor sae2. this modification is conserved from yeast to humans,and is induced by dna damage. we mapped the sumoylation site of sae2 to a single lysine in its self-association domain. abolishing sae2 sumoylation by mutating this lysine to arginine impaired sae2 function in the processing and repair of multiple types of dna breaks. we found that sae2 sumoylation occurs independently of its phosphorylation,and the two modifications act in synergy to increase soluble forms of sae2. we also provide evidence that sumoylation of the sae2-binding nuclease,the mre11-rad50-xrs2 complex,further increases end resection. these findings reveal a novel role for sumoylation in dna repair by regulating the solubility of an end resection factor. they also show that collaboration between different modifications and among multiple substrates leads to a stronger biological effect. © 2015 sarangi et al.
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آدرس
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molecular biology program,memorial sloan-kettering cancer center,new york,ny,united states,programs in biochemistry,cell,and molecular biology,weill cornell graduate school of medical sciences,new york,ny, United States, department of biochemistry,university of oxford,oxford, United Kingdom, department of biology,masaryk university,brno, Czech Republic, howard hughes medical institute,department of molecular biosciences,and institute for cellular and molecular biology,university of texas at austin,austin,tx, United States, howard hughes medical institute,department of molecular biosciences,and institute for cellular and molecular biology,university of texas at austin,austin,tx, United States, department of biology,masaryk university,brno,czech republic,national centre for biomolecular research,masaryk university,brno,czech republic,international clinical research center,st. anne's university hospital in brno,brno, Czech Republic, department of biochemistry,university of oxford,oxford, United Kingdom, molecular biology program,memorial sloan-kettering cancer center,new york,ny,united states,programs in biochemistry,cell,and molecular biology,weill cornell graduate school of medical sciences,new york,ny, United States
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Authors
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