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首页> 外文期刊>Clinical Endocrinology >Effects of up to 15 years of recombinant human GH (rhGH) replacement on bone metabolism in adults with Growth Hormone Deficiency (GHD): The Leiden Cohort Study
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Effects of up to 15 years of recombinant human GH (rhGH) replacement on bone metabolism in adults with Growth Hormone Deficiency (GHD): The Leiden Cohort Study

机译:长达15年的重组人GH(rhGH)替代对生长激素缺乏症(GHD)成人的骨代谢的影响:莱顿队列研究

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摘要

Background Growth hormone deficiency (GHD) in adulthood may be associated with a decreased bone mineral density (BMD), a decreased bone mineral content (BMC) and an increased fracture risk. Recombinant human GH (rhGH) replacement induces a progressive increase in BMD for up to 5-7 years of treatment. Data on longer follow-up are, however, scarce.Methods Two hundred and thirty-adult GHD patients (mean age 47·1 years, 52·6% female), of whom 88% patients had adult-onset (AO) GHD, receiving rhGH replacement for ≥5 years were included in the study. Most patients had multiple pituitary hormone deficiencies. Bone turnover markers, BMC and BMD and T-scores at the lumbar spine and femoral neck were evaluated at baseline, and after 5, 10 and 15 years of rhGH replacement. In addition, clinical fracture incidence was assessed.Results Mean lumbar spine BMD, lumbar spine BMC and T-scores gradually increased during the first 10 years of rhGH replacement and remained stable thereafter. Largest effects of rhGH supplementation were found in men. In the small subset of patients using bisphosphonates, use of bisphosphonates did not impact additional beneficial effects in the long term. Low baseline BMD positively affected the change in BMD and BMC over time, but there was a negative effect of high GH dose at 1 year on the change in BMD and BMC over time. Clinical fracture incidence during long-term rhGH replacement was 20.1/1000 py.Conclusions Fifteen years of rhGH replacement in GHD adults resulted in a sustained increase in BMD values at the lumbar spine, particularly in men, and stabilization of BMD values at the femoral neck. Clinical fracture incidence was suggested not to be increased during long-term rhGH replacement.
机译:背景成年期生长激素缺乏症(GHD)可能与骨矿物质密度(BMD)降低,骨矿物质含量(BMC)降低以及骨折风险增加有关。重组人GH(rhGH)替代可在长达5-7年的治疗中诱导BMD逐渐增加。方法230例成人GHD患者(平均年龄47·1岁,女性52·6%),其中88%患者患有成人GHD,接受≥5年rhGH替代治疗的患者包括在研究中。大多数患者患有多种垂体激素缺乏症。在基线以及rhGH替代治疗5、10和15年后,评估腰椎和股骨颈的骨转换标记,BMC和BMD以及T分数。此外,还评估了临床骨折发生率。结果:rhGH替换的前10年,平均腰椎BMD,腰椎BMC和T评分逐渐升高,此后保持稳定。补充rhGH的最大作用是在男性中。在使用双膦酸盐的小部分患者中,双膦酸盐的长期使用不会影响其他有益效果。低基线BMD对BMD和BMC随时间的变化具有积极影响,但1年时高GH剂量对BMD和BMC随时间的变化具有负面影响。长期rhGH置换期间临床骨折发生率为20.1 / 1000 py。结论在GHD成人中十五年rhGH置换导致腰椎(尤其是男性)的BMD值持续升高,并使股骨颈的BMD值稳定。建议长期rhGH替代期间不增加临床骨折发生率。

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