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SAT-033 U-Shaped Association of Plasma Testosterone and No Association of Plasma Estradiol with Incidence of Any Fracture and Hip Fracture in Older Men

机译:SAT-033血浆睾酮的U形睾酮和血浆雌二醇和血浆雌二醇的关联在老年人的任何骨折和髋部骨折的发生率

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摘要

Osteoporosis resulting in bone fractures is a major cause of morbidity in older men. Previous studies implicated reduced exposure to estradiol (E2) with increased fracture risk in men. The extent to which circulating androgens contribute to maintenance of bone health is uncertain. We examined associations of different sex hormones with incidence of any bone fracture or hip fracture in older men. We analysed 3,307 community-dwelling men aged 76.8±3.5 years, median follow-up period of 10.6 years. Medical information was collected by questionnaire. Frailty was assessed using the FRAIL scale (1). Early morning plasma testosterone (T), dihydrotestosterone (DHT) and E2 were assayed by mass spectrometry, sex hormone-binding globulin (SHBG) and luteinising hormone (LH) by immunoassay. Incidence of any fracture and hip fracture were determined via data linkage to emergency department presentations and hospital admissions. Risk of fracture according to sex hormone concentrations was analysed. Hazard ratio of fracture according to sex hormone quartiles (Q1-4) was assessed using Cox regression models adjusted for age, medical comorbidities and frailty. In 30,355 participant-years of follow-up, the incidence of any fracture was 1.1% and hip fracture 0.5% per participant per year. Incident fractures occurred in 330 men, including 144 hip fractures. Probability plots suggested non-linear relationships between hormones and risk of any fracture and hip fracture, with higher risk at lower and higher concentrations of plasma T, lower E2, higher SHBG and higher LH. In fully-adjusted models, there was a U-shaped association of plasma T with incidence of any fracture (Q1: reference group, Q2: fully-adjusted hazard ratio [HR]=0.69, 95% confidence interval [CI]=0.51-0.94, p=0.020; Q3: HR=0.59, CI=0.42-0.83, p=0.002; Q4: 0.85, CI=0.62-1.18, p=0.335). A similar U-shaped association of T was found with incidence of hip fracture (Q1: HR=1.0; Q2: HR=0.60, CI=0.37-0.93, p=0.043; Q3: HR=0.52, CI=0.31-0.88, p=0.015; Q4: HR=1.04, CI=0.65-1.68, p=0.866). DHT, E2 and LH were not associated with incidence of any fracture or hip fracture (all p>0.050). SHBG was not associated with incidence of any fracture, but was associated with hip fracture (Q4 vs Q1: HR=1.76, CI=1.05-2.96, p=0.033). In conclusion, we found a non-linear or U-shaped association of T with fracture risk, with no association of E2. Mid-range plasma T was associated with lower incidence of any fracture and hip fracture, and higher SHBG with increased risk of hip fracture. Circulating androgen rather than estrogen may be a biomarker for hormone effects on bone driving fracture risk. A randomised controlled trial of T therapy powered for the outcome of fracture may be warranted and should recruit men with baseline T in the lowest quartile of values. Reference: (1) Hyde Z, et al. J Clin Endocrinol Metab 2010; 95: 3165-3172.
机译:骨质疏松症导致骨折是老年人发病率的主要原因。以前的研究涉及在雌二醇(E2)的暴露下,具有增加的男性的骨折风险。循环雌激素对维持骨骼健康的贡献程度是不确定的。我们检查了不同性激素与老年人任何骨折或髋关节骨折的发病率的关联。我们分析了76.8±3.5岁的3,307名社区住宅男子,中位随访时间为10。6年。问卷收集医疗信息。使用虚线(1)评估脆弱的评估。通过质谱法测定液体血浆睾酮(T),DIHOHOTESTOSTONE(DHT)和E2通过免疫测定,性激素结合球蛋白(SHBG)和旋粉激素(LH)测定。通过数据联系到急诊部门介绍和医院入院的数据联系确定了任何骨折和髋部骨折的发病率。分析了根据性激素浓度的裂缝风险。使用COX回归模型进行评估根据年龄,医疗机理和脆弱的COX回归模型评估骨折的危害比率裂缝(Q1-4)。在30,355名参与者的随访中,任何骨折的发生率为每年每次参与者的1.1%和臀部骨折0.5%。入射骨折发生在330名男性,其中包括144个髋部骨折。概率地块提出了激素与任何骨折和髋部骨折的风险之间的非线性关系,具有较高且较高浓度的血浆T,较低e2,更高的SHBG和更高的LH风险。在完全调整的模型中,存在血浆T的U形血浆T型,具有任何骨折的发生率(Q1:参考组,Q2:完全调整的危险比[HR] = 0.69,95%置信区间[CI] = 0.51- 0.94,P = 0.020; Q3:HR = 0.59,CI = 0.42-0.83,P = 0.002; Q4:0.85,CI = 0.62-1.18,P = 0.335)。发现具有髋部骨折的发生率的类似U形的T型T(Q1:HR = 1.0; Q2:HR = 0.60,CI = 0.37-0.93,P = 0.043; Q3:HR = 0.52,CI = 0.31-0.88, P = 0.015; Q4:HR = 1.04,CI = 0.65-1.68,P = 0.866)。 DHT,E2和LH与任何骨折或髋部骨折的发生率无关(所有P> 0.050)。 SHBG与任何骨折的发生率无关,但与髋部骨折有关(Q4 Vs Q1:HR = 1.76,CI = 1.05-2.96,P = 0.033)。总之,我们发现具有裂缝风险的非线性或U形缔结的T,没有E2关联。中间血浆T与任何骨折和髋部骨折的发病率降低,以及髋部骨折风险增加的SHBG。循环雄激素而不是雌激素可以是用于激素对骨骼裂缝风险的激素作用的生物标志物。可以保证随机对照试验,该治疗用于骨折结果的T治疗,并应在最低的价值观中招募具有基线T的男性。参考:(1)海德Z等人。 J Clin Endocrinol Metab 2010; 95:3165-3172。

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