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Bone density and fractures in Turner syndrome

机译:骨密度和转型综合征中的骨折

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Apparent demineralization of the skeleton has been noted in females with Turner syndrome (TS) since the first descriptions of the disorder. Studies, using quantitative methods to measure areal bone mineral density (BMD) in TS, have often been confounded by small skeletal size and variable exposure to estrogen Recent studies taking bone size into account suggest that BMD at skeletal sites of predominantly trabecular bone, eg, the lumbar spine and ultra distal radius, is normal in women that have used estrogen consistently However, these women have significantly lower than normal BMD at skeletal sites with predominantly cortical bone, e.g., the radial shaft and femoral neck It is unknown whether the reduction in cortical BMD is an intrinsic feature of TS perhaps related to haploinsufficiency for SHOX or another X-linked gene, or due to deficient estrogen exposure during childhood and adolescence, and whether this cortical bone deficit increases fracture risk. Current recommendations to begin low dose estrogen treatment in the early teens may clarify these issues Wide use of bisphosphonates to treat low BMD in young women with TS is not warranted since these agents have little if any effect on cortical bone while trabecular bone has excellent response to estrogens.
机译:由于对这种疾病的第一次描述,骨骼的表观脱蛋白已注意到具有变形综合征(TS)的女性。研究,使用定量方法测量TS中的面骨矿物密度(BMD),经常被小骨骼尺寸和可变暴露于雌激素的暴露于雌激素,以骨骼大小表明,BMD在主要的小梁骨骼的骨骼位点,例如,腰椎和超远端半径是正常的,在患有雌激素的女性始终如一,这些女性在骨骼位点上的正常BMD显着低于骨骼部位,其主要皮质骨骼,例如,径向轴和股骨颈是未知的吗?皮质BMD是TS的内在特征,其特征可能与Shox或其他X链基因的单倍细程,或者由于儿童及青春期期间的雌激素暴露,以及这种皮质骨缺陷是否增加了骨折风险。目前在青少年初期开始低剂量雌激素治疗的建议可以澄清这些问题广泛使用双膦酸盐治疗低BMD在没有保证的年轻女性中,因为这些药剂对皮质骨骼的影响很小,而小梁骨骼的效果很好雌激素。

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