绝经后妇女骨矿物质密度及其与同型半胱氨酸和其他骨生化指标的相关性的评估

R. Verma, Satish Kumar, I. Atam, V. Atam, S. Verma, S. Sonkar, Ajay Kumar, S. Chaudhary
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摘要

介绍-同型半胱氨酸(HCY)防止胶原交联并激活骨内的破骨细胞功能。高同型半胱氨酸血症可能通过组织蛋白酶k影响骨密度(BMD)。目的:探讨骨密度与骨生化指标的相关性。方法:在Hologic QDR1000系统的帮助下,通过DXA扫描研究骨密度。根据世卫组织准则,受试者被分为三个不同的亚组,分别为:骨量正常,骨质减少,骨质疏松。每位受试者进行常规生化实验室检查、HCY、维生素B12和叶酸水平。结果:355名绝经后妇女中,骨质疏松者占69%(245人),骨密度正常者占11.27%(40人),平均年龄(53±8.35岁),骨质减少者占19.72%(70人),平均年龄(52.86±7.93岁)。骨质疏松组患者平均年龄56.49±6.65岁。三组小鼠HCY平均水平分别为15.58±7.92 μmol/L、16.13±7.34μmol/L和17.05±5.13μmol/L。髋部骨密度与年龄呈显著负相关(r=-0.360, p=0.002),而体重与BMI无显著相关。PTH与脊柱(r=-0.0339, p=0.004)、前臂(r=-0.267, p=0.027)和髋关节(r=-0.224, p=0.064)的骨密度呈负相关。结论-低骨密度是绝经后女性患者的重要问题。绝经年龄和持续时间是骨质疏松症发展的独立风险预测因素。维生素D水平不能预测绝经后女性的低骨密度。体重对骨质疏松症有保护作用,尤其是脊柱和前臂骨密度。维生素B12和Hcy水平与低骨密度无关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Estimation of bone mineral density and its correlations with homocysteine, and various other biochemical bone markers in postmenopausal women
Introduction- Omocysteine (HCY) prevents collagen cross-linking and activates osteoclast function within the bones. Bone mineral density (BMD) may be affected by Hyperhomocysteinemia via Cathepsin K. Aim- To find the correlation of BMD with biochemical bone markers. Methods- BMD was investigated by the DXA scan with the help of the Hologic QDR1000 system. As per WHO guidelines, subjects were divided into three different subsets with; normal bone mass, osteopenia, and osteoporosis. Every subject underwent routine biochemical laboratory investigations, HCY, Vitamin B12, and folic acid levels. Results-Among 355 postmenopausal women, 69% (245) had osteoporosis while 11.27% (40) had normal BMD (mean age, 53 ± 8.35 years) and 19.72% (70) had osteopenia (mean age 52.86 ± 7.93 years). The mean age in the osteoporotic group was 56.49 ± 6.65 years. The mean levels of HCY in the three groups were 15.58± 7.92 μmol/L, 16.13± 7.34μmol/L and 17.05± 5.13μmol/L, respectively. Hip BMD showed a strong inverse correlation with age (r=-0.360, p=0.002), while no significant correlations were found between weight and BMI. PTH was consistently seen to be negatively correlated with BMD at Spine (r=-0.0339, p=0.004), Forearm (r=-0.267, p=0.027), and Hip (r=-0.224, p=0.064). Conclusion- Low BMD is an important problem in postmenopausal female patients. Age and duration of menopause are independent risk predictors for the development of osteoporosis. Vitamin D levels do not predict low BMD in postmenopausal females. Weight is protective for osteoporosis especially at spine and forearm BMD. Vitamin B12 and Hcy levels did not correlate with low BMD.
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