Non-histone nuclear protein HMGN2 differently regulates the urothelium barrier function by altering expression of antimicrobial peptides and tight junction protein genes in UPEC J96-infected bladder epithelial cell monolayer

Author:

Tian Hanwen,Miao Junming,Zhang Fumei,Xiong Feng,Zhu Feimei,Li Jinyu,Wang Xiaoying,Chen Shanzhe,Chen Junli,Huang Ning,Wang Yi

Abstract

The urinary tract is vulnerable to frequent challenges from environmental microflora. Uropathogenic Escheri­chia coli (UPEC) makes a major contribution to urinary tract infection (UTI). Previous studies have characterized positive roles of non-histone nuclear protein HMGN2 in lung epithelial innate immune response. In the study presented here, we found HMGN2 expression was up-regulated in UPEC J96-infected urothelium. Surprisingly, over-expression of HMGN2 promoted disruption of BECs 5637 cells’ intercellular junctions by down-regulating tight junction (TJs) components’ expression and physi­cal structure under J96 infection. Further investigation showed that BECs 5637 monolayer, in which HMGN2 was over-expressed, had significantly increased permeability to J96. Our study systemically explored the regulatory roles of HMGN2 in BECs barrier function during UPEC infection and suggested different modulations of intra­cellular and paracellular routes through which UPEC in­vades the bladder epithelium.

Publisher

Polskie Towarzystwo Biochemiczne (Polish Biochemical Society)

Subject

General Biochemistry, Genetics and Molecular Biology

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