Haploinsufficiency of Tmem43 in cardiac myocytes activates the DNA damage response pathway leading to a late-onset senescence-associated pro-fibrotic cardiomyopathy.

Leila RouhiSirisha M CheedipudiSuet Nee ChenSiyang FanRaffaella LombardiXiaofan ChenCristian CoarfaMatthew J RobertsonPriyatansh GurhaAli J Marian

Published in: Cardiovascular research (2022)

TMEM43 haploinsufficiency is associated with activation of the DDR and the TP53 pathways, which lead to increased expression of SASP and an age-dependent expression of a pro-fibrotic cardiomyopathy. Given that TMEM43 is a nuclear envelope protein and our previous data showing deficiency of another nuclear envelope protein, namely lamin A/C, activates the DDR/TP53 pathway, we surmise that DNA damage is a shared mechanism in the pathogenesis of cardiomyopathies caused by mutations involving nuclear envelope proteins.

Keyphrases

late onset
dna damage
dna damage response
poor prognosis
binding protein
dna repair
early onset
heart failure
systemic sclerosis
idiopathic pulmonary fibrosis
anti inflammatory
oxidative stress
protein protein
amino acid
endothelial cells
artificial intelligence
deep learning
replacement therapy