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Bacteria-to-Human Protein Networks Reveal Origins of Endogenous DNA Damage.

Cell. 2019-01; 
XiaJun,ChiuLi-Ya,NehringRalf B,Bravo Nú?ezMaría Angélica,MeiQian,PerezMercedes,ZhaiYin,FitzgeraldDevon M,PribisJohn P,WangYumeng,HuChenyue W,PowellReid T,LaBonteSandra A,JalaliAli,Matadamas GuzmánMeztli L,LentzschAlfred M,SzafranAdam T,JoshiMohan C,RichtersMegan,GibsonJanet L,FrischRyan L,HastingsP J,BatesDavid,QueitschChristine,HilsenbeckSusan G,CoarfaCristian,HuJames C,SiegeleDeborah A,ScottKenneth L,LiangHan,ManciniMichael A,HermanChristophe,MillerKyle M,RosenbergSus
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摘要

DNA damage provokes mutations and cancer and results from external carcinogens or endogenous cellular processes. However, the intrinsic instigators of endogenous DNA damage are poorly understood. Here, we identify proteins that promote endogenous DNA damage when overproduced: the DNA "damage-up" proteins (DDPs). We discover a large network of DDPs in Escherichia coli and deconvolute them into six function clusters, demonstrating DDP mechanisms in three: reactive oxygen increase by transmembrane transporters, chromosome loss by replisome binding, and replication stalling by transcription factors. Their 284 human homologs are over-represented among known cancer drivers, and their RNAs in tumors predic... More

关键词

DNA damage response,DNA double-strand breaks,DNMT1,Escherichia coli,cancer,evolution,genome instability,human cells,microbial cancer models,replication fork reve