Back to Search Start Over

PAR2‐mediated cellular senescence promotes inflammation and fibrosis in aging and chronic kidney disease.

Authors :
Ha, Sugyeong
Kim, Hyun Woo
Kim, Kyung Mok
Kim, Byeong Moo
Kim, Jeongwon
Son, Minjung
Kim, Doyeon
Kim, Mi‐Jeong
Yoo, Jian
Yu, Hak Sun
Jung, Young‐Suk
Lee, Jaewon
Chung, Hae Young
Chung, Ki Wung
Source :
Aging Cell; Aug2024, Vol. 23 Issue 8, p1-16, 16p
Publication Year :
2024

Abstract

Cellular senescence contributes to inflammatory kidney disease via the secretion of inflammatory and profibrotic factors. Protease‐activating receptor 2 (PAR2) is a key regulator of inflammation in kidney diseases. However, the relationship between PAR2 and cellular senescence in kidney disease has not yet been described. In this study, we found that PAR2‐mediated metabolic changes in renal tubular epithelial cells induced cellular senescence and increased inflammatory responses. Using an aging and renal injury model, PAR2 expression was shown to be associated with cellular senescence. Under in vitro conditions in NRK52E cells, PAR2 activation induces tubular epithelial cell senescence and senescent cells showed defective fatty acid oxidation (FAO). Cpt1α inhibition showed similar senescent phenotype in the cells, implicating the important role of defective FAO in senescence. Finally, we subjected mice lacking PAR2 to aging and renal injury. PAR2‐deficient kidneys are protected from adenine‐ and cisplatin‐induced renal fibrosis and injury, respectively, by reducing senescence and inflammation. Moreover, kidneys lacking PAR2 exhibited reduced numbers of senescent cells and inflammation during aging. These findings offer fresh insights into the mechanisms underlying renal senescence and indicate that targeting PAR2 or FAO may be a promising therapeutic approach for managing kidney injury. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
14749718
Volume :
23
Issue :
8
Database :
Complementary Index
Journal :
Aging Cell
Publication Type :
Academic Journal
Accession number :
178994720
Full Text :
https://doi.org/10.1111/acel.14184