Hdac1 and Hdac2 positively regulate Notch1 gain-of-function pathogenic signaling in committed osteoblasts of male mice.

Haydee M TorresLeetoria HinojosaAshley M VanCleaveTania RodeznoJennifer J WestendorfJianning Tao

Published in: Birth defects research (2023)

These results provide evidence that Hdac1/2 contribute to Notch1 pathogenic signaling in the mammalian skeleton. Our study on epigenetic regulation of Notch1 GOF-induced osteosclerosis may facilitate further mechanistic studies of skeletal birth defects caused by Notch-related GOF mutations in human patients, such as Adams-Oliver disease, congenital heart disease, and lateral meningocele syndrome.

Keyphrases

congenital heart disease
cell proliferation
histone deacetylase
end stage renal disease
endothelial cells
newly diagnosed
ejection fraction
chronic kidney disease
high glucose
prognostic factors
drug induced
case report
diabetic rats
gestational age
preterm birth
pluripotent stem cells