Cardioprotective response and senescence in aged sEH null female mice exposed to LPS.
Ala YousefDeanna K SosnowskiLiye FangRenald James LegaspiJacob KorodimasAndy LeeKatharine E MagorJohn M SeubertPublished in: American journal of physiology. Heart and circulatory physiology (2024)
Deterioration of physiological systems, like the cardiovascular system, occurs progressively with age impacting an individual's health and increasing susceptibility to injury and disease. Cellular senescence has an underlying role in age-related alterations and can be triggered by natural aging or prematurely by stressors such as the bacterial toxin lipopolysaccharide (LPS). The metabolism of polyunsaturated fatty acids by CYP450 enzymes produces numerous bioactive lipid mediators that can be further metabolized by soluble epoxide hydrolase (sEH) into diol metabolites, often with reduced biological effects. In our study, we observed age-related cardiac differences in female mice, where young mice demonstrated resistance to LPS injury, and genetic deletion or pharmacological inhibition of sEH using trans -4-[4-(3-adamantan-1- yl -ureido)-cyclohexyloxy]-benzoic acid attenuated LPS-induced cardiac dysfunction in aged female mice. Bulk RNA-sequencing analyses revealed transcriptomics differences in aged female hearts. The confirmatory analysis demonstrated changes to inflammatory and senescence gene markers such as Il-6 , Mcp1 , Il-1β , Nlrp3 , p21 , p16 , SA-β-gal , and Gdf15 were attenuated in the hearts of aged female mice where sEH was deleted or inhibited. Collectively, these findings highlight the role of sEH in modulating the aging process of the heart, whereby targeting sEH is cardioprotective. NEW & NOTEWORTHY Soluble epoxide hydrolase (sEH) is an essential enzyme for converting epoxy fatty acids to their less bioactive diols. Our study suggests deletion or inhibition of sEH impacts the aging process in the hearts of female mice resulting in cardioprotection. Data indicate targeting sEH limits inflammation, preserves mitochondria, and alters cellular senescence in the aged female heart.
Keyphrases
- high fat diet induced
- inflammatory response
- lps induced
- dna damage
- heart failure
- oxidative stress
- healthcare
- endothelial cells
- fatty acid
- escherichia coli
- public health
- single cell
- type diabetes
- metabolic syndrome
- mental health
- drug delivery
- signaling pathway
- stress induced
- machine learning
- genome wide
- gene expression
- artificial intelligence
- cell death
- copy number
- toll like receptor
- health information
- adipose tissue
- big data
- electronic health record
- middle aged