睾酮可增加女性向男性跨性别者的骨矿物质密度:15例病例系列研究
Testosterone increases bone mineral density in female-to-male transsexuals: a case series of 15 subjects.
作者信息
Turner Adrian, Chen Tai C, Barber Tom W, Malabanan Alan O, Holick Michael F, Tangpricha Vin
机构信息
Boston University School of Medicine, Department of Medicine, Section of Endocrinology, Diabetes and Nutrition, Boston, Massachusetts, USA.
出版信息
Clin Endocrinol (Oxf). 2004 Nov;61(5):560-6. doi: 10.1111/j.1365-2265.2004.02125.x.
OBJECTIVE
Testosterone therapy for osteoporosis has not been studied extensively in women because of its potential to cause virilization. Female-to-male transsexuals are genetic females who suffer from gender dysphoria and thus take supra-physiologic doses of testosterone to change from the female to male phenotype. The aim of this study is to examine the effects of testosterone treatment on the genetic female skeleton.
PATIENTS AND DESIGN
A group of 15 female-to-male transsexuals was prospectively enrolled for observation over a 2-year period. The subjects had a mean age of 37.0 +/- 3.0 years. All of the subjects self-administered testosterone esters intramuscularly at a mean dose of 70.7 +/- 4.5 mg weekly.
MEASUREMENTS
The subjects had measurements of bone mineral density (BMD) by dual X-ray absorptiometry (DXA) of the femoral neck and spine (L2-L4) at 12-month intervals. They had determinations of serum oestradiol, testosterone, soluble RANKL (sRANKL), osteoprotegerin (OPG) and urine N-telopeptide (NTX) at the date of enrolment and at the end of 2 years. results There was a significant positive increase in mean BMD of 7.8% at the femoral neck and a nonsignificant increase in mean BMD of 3.1% at the spine over 2 years. The levels of testosterone reached the upper normal range for males and the levels of oestradiol declined to near the postmenopausal range. sRANKL levels decreased significantly in female-to-male transsexuals who newly initiated testosterone therapy. There was no significant change in urine NTX or serum OPG during the study.
CONCLUSIONS
We conclude that supra-physiologic testosterone therapy increases BMD at the hip while maintaining BMD at the spine in female-to-male transsexuals. The effects of testosterone may be the result of testosterone hormone directly acting on the bone or indirectly through aromatization to oestradiol. Lower RANKL levels coupled with unchanged OPG levels results in an increased OPG/RANKL ratio, which may be beneficial to the bone by inhibiting osteoclastogenesis.
目的
由于睾酮治疗骨质疏松症可能导致男性化,因此尚未在女性中进行广泛研究。女变男的变性者是患有性别焦虑症的遗传女性,因此会服用超生理剂量的睾酮以从女性表型转变为男性表型。本研究的目的是研究睾酮治疗对遗传女性骨骼的影响。
患者与设计
前瞻性纳入一组15名女变男的变性者,进行为期2年的观察。受试者的平均年龄为37.0±3.0岁。所有受试者均自行肌肉注射睾酮酯,平均剂量为每周70.7±4.5毫克。
测量
受试者每隔12个月通过双能X线吸收法(DXA)测量股骨颈和脊柱(L2-L4)的骨密度(BMD)。在入组时和2年结束时测定血清雌二醇、睾酮、可溶性核因子κB受体活化因子配体(sRANKL)、骨保护素(OPG)和尿N-端肽(NTX)。结果在2年期间,股骨颈平均骨密度显著正性增加7.8%,脊柱平均骨密度非显著性增加3.1%。睾酮水平达到男性正常范围上限,雌二醇水平降至接近绝经后范围。新开始睾酮治疗的女变男变性者的sRANKL水平显著降低。研究期间尿NTX或血清OPG无显著变化。
结论
我们得出结论,超生理剂量的睾酮治疗可增加女变男变性者髋部的骨密度,同时维持脊柱的骨密度。睾酮的作用可能是睾酮激素直接作用于骨骼,或通过芳香化转化为雌二醇间接作用的结果。较低的RANKL水平与不变的OPG水平导致OPG/RANKL比值增加,这可能通过抑制破骨细胞生成而对骨骼有益。
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