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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Apolipoprotein E polymorphism: A new genetic marker of hip fracture risk--The Study of Osteoporotic Fractures.
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Apolipoprotein E polymorphism: A new genetic marker of hip fracture risk--The Study of Osteoporotic Fractures.

机译:载脂蛋白E多态性:髋部骨折风险的新遗传标记-骨质疏松性骨折的研究。

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摘要

Hip fractures are common and devastating events. The apolipoprotein E*4 (APOE) allele, associated with Alzheimer's disease, has also been associated with osteoporosis in hemodialysis patients. We prospectively studied 1750 women, age >/=65 years, who underwent measurements of hip and calcaneal bone mineral density (BMD), were typed for APOE and followed for approximately 7.0 years for the occurrence of fractures and falls. Women with at least one APOE*4 allele had an increased risk of hip fracture, relative hazard (RH) (95% confidence interval) = 1.90 (1.05-3.41) and wrist fracture, RH = 1.67 (1.01-2.77) compared with women without APOE*4, even after adjusting for age, cognitive function, falling, and BMD. The effect of APOE*4 on hip fracture was greatest among women with additional (>/=3) other risk factors. Women with an APOE*4 allele were also likely to report a maternal history of fracture. The average number of falls per year did not differ by APOE*4: 0.46 for APOE*4 women and 0.41 for women without an APOE*4 allele. Women with an APOE*4 allele experienced greater weight loss which contributed to faster rates of bone loss. We conclude that women with the APOE*4 polymorphism are at substantially increased risk of hip and wrist fracture that is not explained by bone density, impaired cognitive function, or falling. Possible alternate explanations include an effect of APOE on vitamin K, bone turnover, or weight loss. The APOE polymorphism may be a candidate gene for hip fractures among community dwelling nondemented women.
机译:髋部骨折是常见的破坏性事件。与阿尔茨海默氏病相关的载脂蛋白E * 4(APOE)等位基因也与血液透析患者的骨质疏松症相关。我们前瞻性地研究了1750名年龄在65岁以上的女性,这些女性接受了髋骨和跟骨骨矿物质密度(BMD)的测量,被确定为APOE类型,然后随访大约7.0年才发生骨折和跌倒。与女性相比,具有至少一个APOE * 4等位基因的女性发生髋部骨折,相对危险(RH)(95%置信区间)= 1.90(1.05-3.41)和腕部骨折,RH = 1.67(1.01-2.77)的风险增加即使调整了年龄,认知功能,跌倒和BMD,也没有APOE * 4。具有其他(> / = 3)其他危险因素的女性中,APOE * 4对髋部骨折的影响最大。具有APOE * 4等位基因的女性也可能报告了母亲的骨折史。 APOE * 4每年的平均跌倒次数没有差异:APOE * 4妇女为0.46,无APOE * 4等位基因的妇女为0.41。具有APOE * 4等位基因的女性体重减轻更大,这有助于更快地减少骨质流失。我们得出的结论是,具有APOE * 4多态性的女性患髋部和腕部骨折的风险显着增加,而这不能通过骨密度,认知功能受损或跌倒来解释。可能的替代解释包括APOE对维生素K,骨骼更新或体重减轻的影响。 APOE基因多态性可能是居住在社区的非痴呆妇女中髋部骨折的候选基因。

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