PER2 is downregulated by the LPS-induced inflammatory response in synoviocytes in rheumatoid arthritis and is implicated in disease susceptibility
- Abstract
- The clinical symptoms of rheumatoid arthritis (RA) present with circadian variation, with joint stiffness and pain more prominent in the early morning. The mammalian clock genes, which include circadian locomotor output cycles kaput, brain and muscle Arnt-like protein 1, period and cryptochrome, regulate circadian rhythms. In order to identify the association between genetic polymorphisms in the circadian clock gene period2 (PER2) and RA, the present study genotyped three PER2 single nucleotide polymorphisms (SNPs), rs934945, rs6754875, and rs2304674, using genetic information from 256RA patients and 499control subjects. Primary cultured rheumatoid synovial cells were stimulated with 10µM lipopolysaccharide (LPS). Total protein was then extracted from the synovial cells following 12and24h, and PER2 protein expression was assayed by immunoblotting. The rs2304674 SNP demonstrated a significant association with susceptibility to RA following Bonferroni correction. However, statistical analysis indicated that the SNPs were not associated with any clinical features of patients with RA. Immunoblotting analysis demonstrated that PER2 protein expression was decreased by LPS‑induced inflammation in RA synovial cells; however, this was not observed in normal synovial cells. The results suggest that the PER2 gene may be a risk factor for RA, and expression of the PER2 protein may be affected by inflammation. Therefore, PER2 may contribute to the pathogenesis of RA.
- All Author(s)
- H. Lee
; S. S. Nah
; S. H. Chang
; H. K. Kim
; J. T. Kwon
; S. Lee
; I. H. Cho
; S. W. Lee
; Y. O. Kim
; S. J. Hong
; H. J. Kim
- Issued Date
- 2017
- Type
- Article
- Keyword
- rheumatoid arthritis; synoviocytes; polymorphism; period 2 gene; association
- Publisher
- D. A. Spandidos
- ISSN
- 1791-2997
; 1791-3004
- Citation Title
- Molecular medicine reports
- Citation Volume
- 16
- Citation Number
- 1
- Citation Start Page
- 422
- Citation End Page
- 428
- Language(ISO)
- eng
- DOI
- 10.3892/mmr.2017.6578
- URI
- http://schca-ir.schmc.ac.kr/handle/2022.oak/2467
- 공개 및 라이선스
-
- 파일 목록
-
Items in Repository are protected by copyright, with all rights reserved, unless otherwise indicated.