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Dipeptidyl peptidase 9 triggers BRCA2 degradationand promotes DNA damage repair

EMBO Rep. 2022-08; 
Oguz Bolgi 1 2, Maria Silva-Garcia 2, Breyan Ross 3 4, Esther Pilla 2, Vijayalakshmi Kari 5, Markus Killisch 2, Melanie Spitzner 5, Nadine Stark 6, Christof Lenz 7 8, Konstantin Weiss 9, Laura Donzelli 1, Mark D Gorrell 10, Marian Grade 5, Jan Riemer 9, Henning Urlaub 7 8, Matthias Dobbelstein 6, Robert Huber 3 11 12, Ruth Geiss-Friedlander 1 2
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Peptide Synthesis BRCA21-1000 in pcDNA3.1(+) P2A eGFP( Genscript) Get A Quote

摘要

N-terminal sequences are important sites for post-translational modifications that alter protein localization, activity, and stability. Dipeptidyl peptidase 9 (DPP9) is a serine aminopeptidase with the rare ability to cleave off N-terminal dipeptides with imino acid proline in the second position. Here, we identify the tumor-suppressor BRCA2 as a DPP9 substrate and show this interaction to be induced by DNA damage. We present crystallographic structures documenting intracrystalline enzymatic activity of DPP9, with the N-terminal Met1-Pro2 of a BRCA21-40 peptide captured in its active site. Intriguingly, DPP9-depleted cells are hypersensitive to genotoxic agents and are impaired in the repair of DNA double-stran... More

關鍵詞

BRCA2; DNA repair; DPP9; N-degron; proteolysis.
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