Ectopic bone formation and systemic bone loss in a transmembrane TNF-driven model of human spondyloarthritis.

Eleni Christodoulou-VafeiadouChristina GekaLydia NtariKsanthi KranidiotiEleni ArgyropoulouFlorian MeierMarietta ArmakaIordanis MourouzisConstantinos PantosMaritina RouchotaGeorge LoudosMaria C DenisNiki KaragianniGeorge Kollias

Published in: Arthritis research & therapy (2020)

The TgA86 mice develop a spontaneous peripheral and axial biphasic pathology accompanied by comorbid heart valvular dysfunction and osteoporosis, overall reproducing the progression of pathognomonic features of human spondyloarthritis. Therefore, the TgA86 mouse represents a valuable model for deciphering the role of transmembrane TNF in the pathogenic mechanisms of spondyloarthritis and for assessing the efficacy of human therapeutics targeting different phases of the disease.

Keyphrases

endothelial cells
ankylosing spondylitis
induced pluripotent stem cells
rheumatoid arthritis
disease activity
pluripotent stem cells
bone loss
heart failure
atrial fibrillation
type diabetes
small molecule
systemic lupus erythematosus
body composition
high fat diet induced