Høst Christian, Christiansen Jens J, Christiansen Jens S, Jorgensen Jens O L, Gravholt Claus H
Medical Department M, Diabetes and Endocrinology and the Medical Research Laboratories, Clinical Institute, Aarhus University Hospital, DK-8000 Aarhus C, Denmark.
Growth Horm IGF Res. 2010 Feb;20(1):26-30. doi: 10.1016/j.ghir.2009.07.001. Epub 2009 Aug 5.
Hypopituitarism, often characterized by hypogonadism, is associated with central obesity, increased cardiovascular and endocrine morbidity and mortality. In Turner syndrome, which is also characterized by hypogonadism liver enzymes are often elevated, but readily suppressed by a short course of hormone replacement therapy (HRT). We investigated the effect of HRT on liver enzymes, lipid levels and measures of insulin sensitivity 26 in hypopituitary women.
We studied 26 hypopituitary women (age 38.8+/-11.0 (mean+/-SD years), BMI 27.4+/-5.1kg/m(2)) during HRT and 28days off therapy.
We measured liver enzymes, fasting levels of lipids, insulin and glucose as well as adiponectin and leptin levels. Body composition was assessed by means of anthropometry and bioimpedance.
Alanine transaminase (ALT) and aspartate transaminase (AST) increased after discontinuation of HRT (ALT; treated: 22.3+/-11.5 vs. untreated: 27.1+/-11.1 (U/L) (P<0.02); AST; treated: 20.4+/-6.1 vs. untreated: 24.6+/-8.9 (U/L) (P<0.002)), whereas other liver function tests remained unchanged. Measures of insulin sensitivity and fasting lipids were also unaffected by HRT, whereas leptin levels decreased with cessation of HRT (leptin; treated: 23 (8-71) vs. untreated: 20 (8-64) (mug/L) (P<0.0005)).
Short time discontinuation of HRT in young hypopituitary women increased liver enzymes, whereas measures of insulin sensitivity and lipid levels remained unchanged. We speculate that the estrogen component of HRT has beneficial effects on hepatic metabolism through various pathways. Further studies including liver imaging and with a time-dependent design are needed to clarify the role of HRT on liver enzyme levels, metabolic variables and liver fat content.
垂体功能减退常以性腺功能减退为特征,与中心性肥胖、心血管和内分泌疾病发病率及死亡率增加相关。在同样以性腺功能减退为特征的特纳综合征中,肝酶常升高,但短期激素替代疗法(HRT)可使其迅速降低。我们研究了HRT对垂体功能减退女性肝酶、血脂水平及胰岛素敏感性指标的影响。
我们对26名垂体功能减退女性(年龄38.8±11.0(平均±标准差岁),体重指数27.4±5.1kg/m²)在接受HRT期间及停药28天时进行了研究。
我们测量了肝酶、空腹血脂、胰岛素和血糖水平以及脂联素和瘦素水平。通过人体测量和生物电阻抗评估身体成分。
停用HRT后丙氨酸转氨酶(ALT)和天冬氨酸转氨酶(AST)升高(ALT;治疗组:22.3±11.5 vs.未治疗组:27.1±11.1(U/L)(P<0.02);AST;治疗组:20.4±6.1 vs.未治疗组:24.6±8.9(U/L)(P<0.002)),而其他肝功能检查保持不变。胰岛素敏感性指标和空腹血脂也不受HRT影响,而瘦素水平随HRT停药而降低(瘦素;治疗组:23(8 - 71)vs.未治疗组:20(8 - 64)(μg/L)(P<0.0005))。
年轻垂体功能减退女性短期停用HRT会使肝酶升高,而胰岛素敏感性指标和血脂水平保持不变。我们推测HRT中的雌激素成分通过多种途径对肝脏代谢有有益作用。需要进一步开展包括肝脏成像及采用时间依赖性设计的研究,以阐明HRT对肝酶水平、代谢变量和肝脏脂肪含量的作用。
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