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首页> 外文期刊>The journal of clinical endocrinology and metabolism >Serum Thyroid-Stimulating Hormone Concentration and Morbidity from Cardiovascular Disease and Fractures in Patients on Long-Term Thyroxine Therapy
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Serum Thyroid-Stimulating Hormone Concentration and Morbidity from Cardiovascular Disease and Fractures in Patients on Long-Term Thyroxine Therapy

机译:长期接受甲状腺素治疗的患者的心血管疾病和骨折引起的血清促甲状腺激素浓度和发病率

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Context: For patients on T_(4) replacement, the dose is guided by serum TSH concentrations, but some patients request higher doses due to adverse symptoms.Objective: The aim of the study was to determine the safety of patients having a low but not suppressed serum TSH when receiving long-term T_(4) replacement.Design: We conducted an observational cohort study, using data linkage from regional datasets between 1993 and 2001.Setting: A population-based study of all patients in Tayside, Scotland, was performed.Patients: All patients taking T_(4) replacement therapy (n = 17,684) were included.Main Outcome Measures: Fatal and nonfatal endpoints were considered for cardiovascular disease, dysrhythmias, and fractures. Patients were categorized as having a suppressed TSH (≤0.03 mU/liter), low TSH (0.04–0.4 mU/liter), normal TSH (0.4–4.0 mU/liter), or raised TSH (>4.0 mU/liter).Results: Cardiovascular disease, dysrhythmias, and fractures were increased in patients with a high TSH: adjusted hazards ratio, 1.95 (1.73–2.21), 1.80 (1.33–2.44), and 1.83 (1.41–2.37), respectively; and patients with a suppressed TSH: 1.37 (1.17–1.60), 1.6 (1.10–2.33), and 2.02 (1.55–2.62), respectively, when compared to patients with a TSH in the laboratory reference range. Patients with a low TSH did not have an increased risk of any of these outcomes [hazards ratio: 1.1 (0.99–1.123), 1.13 (0.88–1.47), and 1.13 (0.92–1.39), respectively].Conclusions: Patients with a high or suppressed TSH had an increased risk of cardiovascular disease, dysrhythmias, and fractures, but patients with a low but unsuppressed TSH did not. It may be safe for patients treated with T_(4) to have a low but not suppressed serum TSH concentration.
机译:背景:对于接受T_(4)替代的患者,剂量应以血清TSH浓度为指导,但某些患者由于不良症状而需要更高剂量。目的:本研究的目的是确定低(但不高)患者的安全性设计:我们采用1993年至2001年间来自区域数据集的数据链接进行了一项观察性队列研究。地点:苏格兰Tayside的所有患者进行的基于人群的研究患者:包括所有接受T_(4)替代疗法的患者(n = 17,684)。主要结果指标:考虑致命和非致命终点的心血管疾病,心律不齐和骨折。患者分为TSH抑制(≤0.03mU /升),TSH低(0.04–0.4 mU /升),TSH正常(0.4–4.0 mU /升)或TSH升高(> 4.0 mU /升)。 :TSH较高的患者的心血管疾病,心律不齐和骨折增加:调整后的危险比分别为1.95(1.73-2.21),1.80(1.33-2.44)和1.83(1.41-2.37);与TSH受抑制的患者相比,TSH在实验室参考范围内的患者分别为1.37(1.17-1.60),1.6(1.10-2.33)和2.02(1.55-2.62)。低TSH的患者没有发生任何上述结果的风险增加[危险比:分别为1.1(0.99-1.123),1.13(0.88-1.47)和1.13(0.92-1.39)]。高TSH或抑制TSH会增加患心血管疾病,心律不齐和骨折的风险,但TSH低但不受抑制的患者则没有。对于接受T_(4)治疗的患者来说,血清TSH浓度较低但并未受到抑制可能是安全的。

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