Bischoff S C, Herrmann A, Göke M, Manns M P, von zur Mühlen A, Brabant G
Department of Gastroenterology & Hepatology, Medical School of Hannover, Germany.
Am J Gastroenterol. 1997 Jul;92(7):1157-63.
A reduced bone mineral density has been reported in inflammatory bowel disease (IBD).
To assess the mechanisms of bone disease in IBD.
We studied in 90 patients (61 with Crohn's disease, 22 with ulcerative colitis, 7 with indeterminate colitis) biochemical markers of bone metabolism in serum and bone mineral density by peripheral quantitative computed tomography at the forearm.
Forty-five percent of the patients had a reduced bone density (Z score < -1). Serum calcium was normal in most patients, vitamin D deficiency was documented in 17%. Osteocalcin, a serum marker of bone formation, was decreased in 26% (1.2 +/- 0.1 ng/ml), whereas the carboxyterminal cross-linked telopeptide of type I collagen (ICTP), a recently described serum parameter of bone breakdown, was stimulated in 38% (10.4 +/- 2.3 microg/L). Of 33 patients with increased ICTP levels, 19 showed a decreased bone density (Z score < -1), and 2 of them never received steroids. An active status of the underlying disease in most patients with increased ICTP levels suggests a direct effect of the underlying IBD. In the whole series of patients with a history of active disease (n = 34), 47% had signs of an increased bone degradation (ICTP > 5 microg/L; mean, 12.9 +/- 4.7 microg/L). Data derived from a retrospective survey of 245 patients with IBD suggest that the prevalence of bone fractures in IBD is unexpectedly high, particularly in patients with a long duration of disease, frequent active phases, and high cumulative doses of corticosteroid intake.
Several mechanisms may be involved in IBD-associated bone disease: (1) a high inflammatory activity directly induces bone degradation via yet unknown pathways, (2) treatment with corticosteroids may exert catabolic effects on the bone, or (3) malabsorption and vitamin D deficiency may activate bone turnover.
据报道,炎症性肠病(IBD)患者骨矿物质密度降低。
评估IBD中骨病的机制。
我们研究了90例患者(61例克罗恩病、22例溃疡性结肠炎、7例未定型结肠炎)血清中骨代谢的生化标志物以及通过前臂外周定量计算机断层扫描测定的骨矿物质密度。
45%的患者骨密度降低(Z值<-1)。大多数患者血清钙正常,17%的患者有维生素D缺乏记录。骨钙素是一种骨形成的血清标志物,26%的患者降低(1.2±0.1 ng/ml),而I型胶原羧基末端交联肽(ICTP)是一种最近描述的骨分解血清参数,38%的患者升高(10.4±2.3 μg/L)。在33例ICTP水平升高的患者中,19例骨密度降低(Z值<-1),其中2例从未接受过类固醇治疗。大多数ICTP水平升高的患者潜在疾病处于活动状态,提示潜在IBD的直接影响。在整个有活动性疾病病史的患者系列(n = 34)中,47%有骨降解增加的迹象(ICTP>5 μg/L;平均值,±4.7 μg/L)。对245例IBD患者的回顾性调查数据表明,IBD中骨折的患病率意外地高,特别是在病程长、频繁活动期和皮质类固醇累积摄入量高的患者中。
IBD相关骨病可能涉及多种机制:(1)高炎症活动通过尚不清楚的途径直接诱导骨降解;(2)皮质类固醇治疗可能对骨产生分解代谢作用;或(3)吸收不良和维生素D缺乏可能激活骨转换。
