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Publication : DNA single-strand break-induced DNA damage response causes heart failure.

First Author  Higo T Year  2017
Journal  Nat Commun Volume  8
Pages  15104 PubMed ID  28436431
Mgi Jnum  J:249553 Mgi Id  MGI:5921321
Doi  10.1038/ncomms15104 Citation  Higo T, et al. (2017) DNA single-strand break-induced DNA damage response causes heart failure. Nat Commun 8:15104
abstractText  The DNA damage response (DDR) plays a pivotal role in maintaining genome integrity. DNA damage and DDR activation are observed in the failing heart, however, the type of DNA damage and its role in the pathogenesis of heart failure remain elusive. Here we show the critical role of DNA single-strand break (SSB) in the pathogenesis of pressure overload-induced heart failure. Accumulation of unrepaired SSB is observed in cardiomyocytes of the failing heart. Unrepaired SSB activates DDR and increases the expression of inflammatory cytokines through NF-kappaB signalling. Pressure overload-induced heart failure is more severe in the mice lacking XRCC1, an essential protein for SSB repair, which is rescued by blocking DDR activation through genetic deletion of ATM, suggesting the causative role of SSB accumulation and DDR activation in the pathogenesis of heart failure. Prevention of SSB accumulation or persistent DDR activation may become a new therapeutic strategy against heart failure.
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