Engvall Inga-Lill, Svensson Björn, Tengstrand Birgitta, Brismar Kerstin, Hafström Ingiäld
Department of Rheumatology, Karolinska Institutet at Karolinska University Hospital Huddinge, Stockholm, Sweden.
Arthritis Res Ther. 2008;10(6):R128. doi: 10.1186/ar2542. Epub 2008 Nov 5.
Patients with rheumatoid arthritis (RA) have an increased frequency of osteoporosis, mainly because of increased bone resorption. Reduction of disease activity is suggested to reduce bone remodelling. It might also be possible that prednisolone treatment could cause this effect because prednisolone has been shown to arrest the development of joint destruction in early RA. Therefore, we examined the effects of low-dose prednisolone on serum concentrations of bone remodelling markers and insulin-like growth factor-1 (IGF-1) in RA patients in relation to bone mineral density.
One hundred and fifty patients, 67% women, with early RA, mean disease duration of six months (95% confidence interval (CI) = three to eight months), who had participated in the BARFOT (Better Anti-Rheumatic FarmacOTherapy) low-dose prednisolone study were included. They had been randomised to either the P-group, who were treated with 7.5 mg prednisolone daily (n = 70, mean age = 51 years, 95% CI 48 to 54 years), or the NoP-group, who received no prednisolone (n = 80, mean age 58 years, 95% CI 56 to 61 years), when they started their first disease-modifying anti-rheumatic drug (DMARD). Serum samples were analysed at baseline, 3 and 12 months for procollagen type I N-terminal propeptide (P1NP), a marker of bone formation, and the C-telopeptide crosslaps of type I collagen (CTX-1) and C-terminal telopeptide of type I collagen (1CTP), markers of bone degradation. IGF-1 was analysed at baseline and after 12 months. Bone mineral density at the lumbar spine and femoral neck was assessed by dual-energy X-ray absorptiometry at baseline and after 24 months.
Levels of P1NP decreased rapidly in the P-group (p < 0.001). Levels of CTX-1 and 1CTP decreased in both treatment groups, but significantly more in the P-group (differences between groups p < 0.019 and p < 0.001, respectively). IGF-1 increased in the P-group (p < 0.001) but remained stable in the NoP-group. Bone mineral density decreased in the spine in both groups, significantly more in postmenopausal women from the P-group. Femur bone mineral density only decreased in the NoP-group.
Low-dose prednisolone in early RA counteracts the negative impact of rheumatoid inflammation on bone tissue in the hip, a juxta-articular localisation. Thus bone mineral density was preserved in the femur in the P-group and 1CTP decreased rapidly. However, the systemic inflammatory consequences on bone could not be prevented in the lumbar spine, especially not in postmenopausal women, probably because of the combined effect of suppression of bone synthesis by prednisolone and the postmenopausal status.
类风湿关节炎(RA)患者骨质疏松的发生率增加,主要是由于骨吸收增加。疾病活动度的降低被认为可减少骨重塑。泼尼松龙治疗也可能产生这种效果,因为泼尼松龙已被证明可阻止早期RA关节破坏的发展。因此,我们研究了低剂量泼尼松龙对RA患者血清骨重塑标志物和胰岛素样生长因子-1(IGF-1)浓度的影响,并将其与骨密度相关联。
纳入150例早期RA患者,其中67%为女性,平均病程6个月(95%置信区间(CI)=3至8个月),这些患者参与了BARFOT(更好的抗风湿药物治疗)低剂量泼尼松龙研究。他们在开始使用第一种改善病情抗风湿药物(DMARD)时被随机分为P组,每日接受7.5mg泼尼松龙治疗(n = 70,平均年龄 = 51岁,95%CI 48至54岁),或NoP组,不接受泼尼松龙治疗(n = 80,平均年龄58岁,95%CI 56至61岁)。在基线、3个月和12个月时分析血清样本,检测骨形成标志物I型前胶原N端前肽(P1NP),以及骨降解标志物I型胶原C端交联肽(CTX-1)和I型胶原C端肽(1CTP)。在基线和12个月后分析IGF-1。在基线和24个月后通过双能X线吸收法评估腰椎和股骨颈的骨密度。
P组中P1NP水平迅速下降(p < 0.001)。两个治疗组中CTX-1和1CTP水平均下降,但P组下降更显著(组间差异分别为p < 0.019和p < 0.001)。P组中IGF-1升高(p < 0.001),而NoP组保持稳定。两组患者脊柱骨密度均下降,P组绝经后女性下降更显著。仅NoP组股骨骨密度下降。
早期RA患者使用低剂量泼尼松龙可抵消类风湿炎症对髋部(关节周围局部)骨组织的负面影响。因此,P组股骨骨密度得以保留,1CTP迅速下降。然而,泼尼松龙抑制骨合成与绝经后状态的联合作用可能导致无法预防腰椎的全身炎症对骨的影响,尤其是在绝经后女性中。
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