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Rett 综合征的 DXA 测量显示骨骼较小,骨量低。

DXA measurements in Rett syndrome reveal small bones with low bone mass.

机构信息

Center for Rett Syndrome, Kennedy Center, Glostrup, Denmark.

出版信息

J Bone Miner Res. 2011 Sep;26(9):2280-6. doi: 10.1002/jbmr.423.

DOI:10.1002/jbmr.423
PMID:21590733
Abstract

Low bone mass is reported in growth-retarded patients harboring mutations in the X-linked methyl-CpG-binding protein 2 (MECP2) gene causing Rett syndrome (RTT). We present the first study addressing both bone mineral density (BMD) and bone size in RTT. Our object was to determine whether patients with RTT do have low BMD when correcting for smaller bones by examination with dual-energy X-ray absorptiometry (DXA). We compared areal BMD (aBMD(spine) and aBMD(total hip) ) and volumetric bone mineral apparent density (vBMAD(spine) and vBMAD(neck) ) in 61 patients and 122 matched healthy controls. Further, spine and hip aBMD and vBMAD of patients were associated with clinical risk factors of low BMD, low-energy fractures, MECP2 mutation groups, and X chromosome inactivation (XCI). Patients with RTT had reduced bone size on the order of 10% and showed lower values of spine and hip aBMD and vBMAD (p < .001) adjusted for age, pubertal status, and body mass index (BMI). aBMD(spine) , vBMAD(spine) , and aBMD(total hip) were associated with low-energy fractures (p < .05). Walking was significantly associated to aBMD(total hip) and vBMAD(neck) adjusted for age and body mass index (BMI). Further, vBMAD(neck) was significantly associated to a diagnosis of epilepsy, antiepileptic treatment, and MECP2 mutation group, but none of the associations with vBMAD(neck) remained clinically significant in a multiple adjusted model including age and BMI. Neither aBMD(spine) , vBMAD(spine) , nor aBMD(total hip) were significantly associated with epilepsy, antiepileptic treatment, MECP2 mutation group, XCI, or vitamin D status. Low bone mass and small bones are evident in RTT, indicating an apparent low-bone-formation phenotype.

摘要

患有 X 连锁甲基化CpG 结合蛋白 2(MECP2)基因突变导致雷特综合征(RTT)的生长迟缓患者报告有低骨量。我们首次研究了 RTT 中的骨密度(BMD)和骨大小。我们的目的是通过双能 X 射线吸收法(DXA)检查,确定 RTT 患者在纠正较小骨骼后是否确实存在低骨密度。我们比较了 61 例患者和 122 例匹配健康对照者的面积 BMD(脊柱 aBMD 和全髋关节 aBMD)和容积骨矿物质表观密度(脊柱 vBMAD 和颈部 vBMAD)。此外,患者的脊柱和髋关节 aBMD 和 vBMAD 与低 BMD、低能量骨折、MECP2 突变组和 X 染色体失活(XCI)的临床危险因素相关。RTT 患者的骨骼大小减少了约 10%,并且脊柱和髋关节的 aBMD 和 vBMAD 降低(p<0.001),经年龄、青春期状态和体重指数(BMI)调整。aBMD(脊柱)、vBMAD(脊柱)和 aBMD(全髋关节)与低能量骨折相关(p<0.05)。行走与经年龄和 BMI 调整的全髋关节 aBMD 和 vBMAD(颈部)显著相关。进一步,vBMAD(颈部)与癫痫诊断、抗癫痫治疗和 MECP2 突变组显著相关,但在包括年龄和 BMI 的多变量调整模型中,vBMAD(颈部)与任何一项的关联均无临床意义。aBMD(脊柱)、vBMAD(脊柱)或 aBMD(全髋关节)均与癫痫、抗癫痫治疗、MECP2 突变组、XCI 或维生素 D 状态无显著相关性。低骨量和小骨骼在 RTT 中明显存在,表明存在明显的低骨形成表型。

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