논문성과

논문성과

Angiotentin receptor blockers, but not angiotensin-converting enzyme inhibitors, inhibit abnormal bone changes in spondyloarthritis
2023-10-18 18:16:42 조회수194
AUTHOR : Choi JS, Kim JY, Ahn MJ, Jang H, Song S, Jo S, Choi SH, Park YS, Kim TH, Shim SC
JOURNAL : Experimental & Molecule Medicine
YEAR : 2023
VOL :
PAGE :

Abstract 

Background 

Spondyloarthritis (SpA) is a chronic inflammatory disease that results in bone ankylosis. The tissue reninangiotensin system (RAS), updated with new components, is an emerging phenomenon possibly implicated in SpA-associated bone changes. Therefore, we sought to determine the mechanism underlying this relationship. 

Methods

Sakaguchi (SKG) mice injected with curdlan (SKGc), animal models for SpA, were treated with the RAS modulators, angiotensin II receptor blockers (ARBs) or angiotensin-converting enzyme inhibitors (ACEis). Disease activity was assessed using clinical scores and computed tomography scans. Mouse primary bone marrow monocytes (BMMs), osteoblast (OB) progenitor cells, peripheral blood monocytes (PBMCs), and bone-derived cells (BdCs) from patients with radiographic axial SpA (r-axSpA) were used to investigate the role of RAS in SpA pathogenesis. 

Results

The expression of RAS components was significantly high in SKGc mouse joints, wherein ARBs significantly reduced erosion and systemic bone loss, whereas ACEis did not. Osteoclast (OC) differentiation from primary BMMs, mediated by TRAF6, was inhibited by ARBs but promoted by ACEis; the modulators also exerted opposite effects on OB differentiation. Expression of RAS molecules was higher in PBMCs and BdCs of patients with r-axSpA than in control participants. ARBs inhibited OB differentiation in the BdCs of patients with r-axSpA, whereas ACEi did not. Neither ARBs nor ACEis affected OB differentiation in the control participants. 

Conclusions

In SpA, a condition characterized by RAS overexpression, ARBs, but not ACEis, inhibited OC and OB differentiation and bone progression. These findings must be considered when treating patients with SpA using RAS modulators. 

 
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