骨骼系统P2受体的功能与炎症性骨疾病

细胞外的嘌呤核苷酸和嘧啶核苷酸作用于P2受体产生生物学效应,P2受体分为P2X和P2Y受体。分子和功能学实验研究表明,骨骼系统的成骨细胞、破骨细胞和软骨细胞有P2X和P2Y受体各种亚型表达。ATP和其他核苷酸释放到骨微环境,与P2受体结合调节骨和软骨的形成和活化,包括生长、发育、重建和修复等各方面的生物学功能。炎症条件下,核苷酸释放增加,刺激破骨细胞的活化和形成。异常的骨重塑可以产生不同的骨骼疾病。P2受体在炎症性骨疾病中起重要作用。

唑来膦酸调控NLRP3信号通路抑制脂多糖诱导的破骨细胞分化

背景:唑来膦酸可抑制骨吸收,但其是否能抑制炎症性骨疾病及其相关机制尚不完全清楚。目的:分析唑来膦酸对脂多糖诱导破骨细胞增殖、分化的影响。方法:利用脂多糖将RAW264.7细胞诱导为破骨细胞,采用抗酒石酸酸性磷酸酶染色和F-actin染色鉴定诱导结果。将RAW264.7细胞分5组培养:空白对照组不进行任何干预,对照组加入脂多糖处理,其余3组在加入脂多糖的基础上分别加入0.1,1,5μmol/L的唑来膦酸处理,培养6 h后,采用ELISA法检测上清液中肿瘤坏死因子α水平,Western Blot检测NLRP3、caspase-1、白细胞介素1β、cleaved-caspase-1及肿瘤坏死因子α的蛋白表达。培养第5天,抗酒石酸酸性磷酸酶染色观察破骨细胞形成情况,F-actin染色观察破骨细胞肌动蛋白环。结果与结论:①抗酒石酸酸性磷酸酶染色和F-actin染色显示,脂多糖可诱导RAW264.7细胞分化为破骨细胞;②对照组肿瘤坏死因子α水平高于空白对照组(P<0.05),0.1,5μmol/L唑来膦酸组肿瘤坏死因子α水平低于对照组(P<0.05);抗酒石酸酸性磷酸酶染色与F-actin染色显示,1,5μmol/L唑来膦酸可抑制脂多糖诱导RAW264.7细胞分化为破骨细胞;③与对照组比较,0.1,1,5μmol/L的唑来膦酸均可抑制NLRP3、caspase-1、白细胞介素1β及肿瘤坏死因子α的蛋白表达(P<0.05),1,5μmol/L的唑来膦酸均可抑制cleaved-caspase-1的蛋白表达(P<0.05);④结果表明,唑来膦酸可抑制脂多糖诱导的破骨细胞分化,该作用可能是通过调控NLRP3信号通路实现的。

Case report： A 10 years follow-up of periprosthetic femoral fracture after total hip arthroplasty in osteopetrosis

Osteopetrosis is an inherited disorder characterized by increased bone density and brittle bone quality. Degenerative changes often occur after the age of 40 in patients with osteopetrosis. Operative inter- vention is the primary treatment option if the clinical manifestation of secondary osteoarthritis is severe. A 44-year-old male suffering autosomal dominant osteopetrosis and progressive unilateral hip osteo- arthritis required a total hip arthroplasty. However, there were several technical challenges associated with this procedure including creating a femoral medullary canal and developing a Vancouver type B2 periprosthetic femoral fracture postoperatively. To afford some experience for the management of similar cases, we here present our technical solutions to these problems.

Cathepsin C promotes the progression of periapical periodontitis

Although the role of cathepsin C (Cat C) in inflammation is gradually being elucidated, its function in periapical periodontitis, which is one of the most common infectious diseases worldwide, has not been studied. This study evaluated a surgically-induced model of periapical periodontitis in cathepsin C (Cat C) knock-down (KD) mice, which was constructed with a tetracycline operator, to evaluate the role of Cat C in the pathogenesis and progression of periapical periodontitis. Our results showed, for the first time, that there was a statistically significant increase in the expression of Cat C as periapical periodontitis progressed;this increase started from 1 week after surgery and reached a peak at 3 weeks after surgery, before gradually decreasing. The volume of periapical bone resorption in Cat C KD mice was significantly smaller than that in wild-type mice at 3 and 4 weeks after surgery (P<0.05). Inflammatory cell infiltration into the apical tissues of wild-type mice was also significantly higher than that of Cat C KD mice. The expression of receptor activator of nuclear factor-j B ligand (RANKL) in wild-type mice was also higher than that in Cat C KD mice. The difference in the number of osteoclasts in the apical area between the two groups was statistically significant after 2 weeks. Correlation analysis showed that there was a significant correlation between Cat C and RANKL expression (r= 0.835). Therefore, our data indicated that Cat C promoted the apical inflammation and bone destruction in mice.