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克莱恩费尔特氏症骨骼微观结构随睾酮替代疗法的演变。

Klinefelter Bone Microarchitecture Evolution with Testosterone Replacement Therapy.

机构信息

Département de Rhumatologie, Hospices Civils de Lyon, Lyon, France.

INSERM UMR 1033, Université de Lyon, Lyon, France.

出版信息

Calcif Tissue Int. 2022 Jul;111(1):35-46. doi: 10.1007/s00223-022-00956-2. Epub 2022 Feb 13.

Abstract

Klinefelter Syndrome (KS) patients, defined by a 47 XXY karyotype, have increased risk of fragility fractures. We have assessed bone microarchitecture by high resolution peripheral quantitative CT (HR-pQCT) at the radius and tibia in young KS patients, naïve from testosterone replacement therapy (TRT). Areal bone mineral density (BMD) and body composition were assessed by dual X-ray absorptiometry (DXA). Total testosterone (tT) was measured at baseline. Bone measurements have been repeated after 30 months of TRT. We enrolled 24 KS patients and 72 age-matched controls. KS patients were (mean ± SD) 23.7 ± 7.8 year-old. KS patients had significantly lower relative appendicular lean mass index (RALM) and lower aBMD at spine and hip than controls. Ten patients (42%) had low tT level (≤ 10.4 nmol/L). At baseline, we observed at radius a marked cortical (Ct) impairment reflected by lower Ct.area, Ct.perimeter, and Ct.vBMD than controls. At tibia, in addition to cortical fragility, we also found significant alterations of trabecular (Tb) compartment with lower trabecular bone volume (BV/TV) and Tb.vBMD as compared to controls. After 30 months of TRT, 18 (75%) KS patients were reassessed. Spine aBMD and RALM significantly increased. At radius, both cortical (Ct.Pm, Ct.Ar, Ct.vBMD, Ct.Th) and trabecular (Tb.vBMD) parameters significantly improved. At tibia, the improvement was found only in the cortical compartment. Young TRT naïve KS patients have inadequate bone microarchitecture at both the radius and tibia, which can improve on TRT.

摘要

克莱恩费尔特综合征(KS)患者的核型为 47 XXY,脆性骨折风险增加。我们通过高分辨率外周定量 CT(HR-pQCT)评估了年轻 KS 患者(未接受过睾酮替代治疗(TRT))桡骨和胫骨的骨微结构。通过双能 X 线吸收法(DXA)评估了骨矿物质密度(BMD)和身体成分。在基线时测量了总睾酮(tT)。在 TRT 治疗 30 个月后重复了骨测量。我们招募了 24 名 KS 患者和 72 名年龄匹配的对照。KS 患者的年龄(平均值±标准差)为 23.7±7.8 岁。KS 患者的相对四肢瘦体重指数(RALM)和脊柱、髋部的 aBMD 明显低于对照组。10 名患者(42%)的 tT 水平较低(≤10.4 nmol/L)。在基线时,我们观察到桡骨的皮质(Ct)明显受损,表现为 Ct.area、Ct.perimeter 和 Ct.vBMD 低于对照组。在胫骨中,除了皮质脆弱外,我们还发现了小梁(Tb)结构的明显改变,与对照组相比,Tb 骨体积(BV/TV)和 Tb.vBMD 较低。在 TRT 治疗 30 个月后,对 18 名(75%)KS 患者进行了重新评估。脊柱 aBMD 和 RALM 显著增加。在桡骨,皮质(Ct.Pm、Ct.Ar、Ct.vBMD、Ct.Th)和小梁(Tb.vBMD)参数均显著改善。在胫骨中,仅在皮质部位观察到改善。年轻的 TRT 初治 KS 患者的桡骨和胫骨均存在骨微结构不足,TRT 可改善这些不足。

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