Expression profiling of genes regulated by sphingosine kinase1 signaling in a murine model of hyperoxia induced neonatal bronchopulmonary dysplasia.

Viswanathan NatarajanAlison W HaYangbasai DongNarsa M ReddyDavid L EbenezerPrasad KantetiSekhar P ReddyJ Usha RajZhengdeng LeiMark Maienschein-ClineZarema ArbievaAnantha Harijith

Published in: BMC genomics (2017)

Using SphK1 knockout mice and differential gene expression analysis, we have shown here that S1P/SphK1 signaling plays a key role in promoting hyperoxia induced DNA damage, inflammation, apoptosis and ECM remodeling in neonatal lungs. It also appears to suppress pro-survival cellular responses involved in normal lung development. We therefore propose SphK1 as a therapeutic target for the development drugs to combat BPD.

Keyphrases

oxidative stress
genome wide identification
dna damage
diabetic rats
genome wide
high glucose
drug induced
endoplasmic reticulum stress
cell death
endothelial cells
copy number
transcription factor
gene expression
dna repair
signaling pathway
tyrosine kinase
free survival