Department of Metabolic Disorders, Amgen Inc, One Amgen Center Drive, Thousand Oaks, CA 91320, USA.
Arthritis Res Ther. 2009;11(6):R187. doi: 10.1186/ar2879. Epub 2009 Dec 11.
Rat adjuvant-induced arthritis (AIA) and collagen-induced arthritis (CIA) feature bone loss and systemic increases in TNFalpha, IL-1beta, and receptor activator of NF-kappaB ligand (RANKL). Anti-IL-1 or anti-TNFalpha therapies consistently reduce inflammation in these models, but systemic bone loss often persists. RANKL inhibition consistently prevents bone loss in both models without reducing joint inflammation. Effects of these therapies on systemic markers of bone turnover and inflammation have not been directly compared.
Lewis rats with established AIA or CIA were treated for 10 days (from day 4 post onset) with either PBS (Veh), TNFalpha inhibitor (pegsunercept), IL-1 inhibitor (anakinra), or RANKL inhibitor (osteoprotegerin (OPG)-Fc). Local inflammation was evaluated by monitoring hind paw swelling. Bone mineral density (BMD) of paws and lumbar vertebrae was assessed by dual X-ray absorptiometry. Markers and mediators of bone resorption (RANKL, tartrate-resistant acid phosphatase 5b (TRACP 5B)) and inflammation (prostaglandin E2 (PGE2), acute-phase protein alpha-1-acid glycoprotein (alpha1AGP), multiple cytokines) were measured in serum (day 14 post onset).
Arthritis progression significantly increased paw swelling and ankle and vertebral BMD loss. Anti-TNFalpha reduced paw swelling in both models, and reduced ankle BMD loss in AIA rats. Anti-IL-1 decreased paw swelling in CIA rats, and reduced ankle BMD loss in both models. Anti-TNFalpha and anti-IL-1 failed to prevent vertebral BMD loss in either model. OPG-Fc reduced BMD loss in ankles and vertebrae in both models, but had no effect on paw swelling. Serum RANKL was elevated in AIA-Veh and CIA-Veh rats. While antiTNFalpha and anti-IL-1 partially normalized serum RANKL without any changes in serum TRACP 5B, OPG-Fc treatment reduced serum TRACP 5B by over 90% in both CIA and AIA rats. CIA-Veh and AIA-Veh rats had increased serum alpha1AGP, IL-1beta, IL-8 and chemokine (C-C motif) ligand 2 (CCL2), and AIA-Veh rats also had significantly greater serum PGE2, TNFalpha and IL-17. Anti-TNFalpha reduced systemic alpha1AGP, CCL2 and PGE2 in AIA rats, while anti-IL-1 decreased systemic alpha1AGP, IL-8 and PGE2. In contrast, RANKL inhibition by OPG-Fc did not lessen systemic cytokine levels in either model.
Anti-TNFalpha or anti-IL-1 therapy inhibited parameters of local and systemic inflammation, and partially reduced local but not systemic bone loss in AIA and CIA rats. RANKL inhibition prevented local and systemic bone loss without significantly inhibiting local or systemic inflammatory parameters.
佐剂诱导的关节炎(AIA)和胶原诱导的关节炎(CIA)具有骨丢失和全身 TNFalpha、IL-1beta 和核因子-kappaB 配体(RANKL)受体激活剂的增加。抗 IL-1 或抗 TNFalpha 治疗可一致减少这些模型中的炎症,但全身骨丢失通常持续存在。RANKL 抑制剂可一致预防两种模型中的骨丢失,而不减少关节炎症。这些治疗方法对系统骨转换和炎症标志物的影响尚未直接比较。
建立 AIA 或 CIA 的 Lewis 大鼠用 PBS(Veh)、TNFalpha 抑制剂(pegsunercept)、IL-1 抑制剂(anakinra)或 RANKL 抑制剂(骨保护素(OPG)-Fc)治疗 10 天(从发病后第 4 天开始)。通过监测后爪肿胀来评估局部炎症。通过双能 X 射线吸收法评估爪子和腰椎的骨密度(BMD)。在发病后第 14 天测量血清中骨吸收标志物和介质(RANKL、抗酒石酸酸性磷酸酶 5b(TRACP 5B))和炎症(前列腺素 E2(PGE2)、急性期蛋白 alpha-1-酸性糖蛋白(alpha1AGP)、多种细胞因子)。
关节炎进展显著增加了爪肿胀和踝关节和椎体 BMD 丢失。抗 TNFalpha 减少了两种模型中的爪肿胀,并减少了 AIA 大鼠的踝关节 BMD 丢失。抗 IL-1 降低了 CIA 大鼠的爪肿胀,并减少了两种模型中的踝关节 BMD 丢失。抗 TNFalpha 和抗 IL-1 未能预防任何模型中的椎体 BMD 丢失。OPG-Fc 减少了两种模型中的踝关节和椎体 BMD 丢失,但对爪肿胀没有影响。AIA-Veh 和 CIA-Veh 大鼠的血清 RANKL 升高。虽然抗 TNFalpha 和抗 IL-1 部分正常化了血清 RANKL,而血清 TRACP 5B 没有任何变化,但 OPG-Fc 治疗使 CIA 和 AIA 大鼠的血清 TRACP 5B 降低了 90%以上。CIA-Veh 和 AIA-Veh 大鼠的血清 alpha1AGP、IL-1beta、IL-8 和趋化因子(C-C 基序)配体 2(CCL2)增加,AIA-Veh 大鼠的血清 PGE2、TNFalpha 和 IL-17 也显著增加。抗 TNFalpha 减少了 AIA 大鼠的全身 alpha1AGP、CCL2 和 PGE2,而抗 IL-1 降低了全身 alpha1AGP、IL-8 和 PGE2。相比之下,OPG-Fc 对 RANKL 的抑制并没有减少两种模型中的全身细胞因子水平。
抗 TNFalpha 或抗 IL-1 治疗抑制了局部和全身炎症的参数,并部分减少了 AIA 和 CIA 大鼠的局部但不包括全身骨丢失。RANKL 抑制可预防局部和全身骨丢失,而不显著抑制局部或全身炎症参数。
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