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Interventions to prevent steroid-induced osteoporosis and osteoporotic fractures in Duchenne muscular dystrophy (Review)

机译:预防类固醇激素引起的骨质疏松症和杜氏肌营养不良的骨折的干预措施(综述)

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摘要

Background: Corticosteroid treatment is considered the 'gold standard' for Duchenne muscular dystrophy (DMD); however, it is also known to induce osteoporosis and thus increase the risk of vertebral fragility fractures. Good practice in the care of those with DMD requires prevention of these adverse effects. Treatments to increase bone mineral density include bisphosphonates and vitamin D and calcium supplements, and in adolescents with pubertal delay, testosterone. Bone health management is an important part of lifelong care for patients with DMD.Objectives: To assess the effects of interventions to prevent or treat osteoporosis in children and adults with DMD taking long-term corticosteroids; to assess the effects of these interventions on the frequency of vertebral fragility fractures and long-bone fractures, and on quality of life; and to assess adverse events.Search methods: On 12 September 2016, we searched the Cochrane Neuromuscular Specialised Register, CENTRAL, MEDLINE, Embase, and CINAHL Plus to identify potentially eligible trials. We also searched the Web of Science ISI Proceedings (2001 to September 2016) and three clinical trials registries to identify unpublished studies and ongoing trials. We contacted correspondence authors of the included studies in the review to obtain information on unpublished studies or work in progress.Selection criteria: We considered for inclusion in the review randomised controlled trials (RCTs) and quasi-RCTs involving any bone health intervention for corticosteroid-induced osteoporosis and fragility fractures in children, adolescents, and adults with a confirmed diagnosis of DMD. The interventions might have included oral and intravenous bisphosphonates, vitamin D supplements, calcium supplements, dietary calcium, testosterone, and weight-bearing activity.Data collection and analysis: Two review authors independently assessed reports and selected potential studies for inclusion, following standard Cochrane methodology. We contacted study authors to obtain further information for clarification on published work, unpublished studies, and work in progress.Main results: We identified 18 potential studies, of which two, currently reported only as abstracts, met the inclusion criteria for this review. Too little information was available for us to present full results or adequately assess risk of bias. The participants were children aged five to 15 years with DMD, ambulant and non-ambulant. The interventions were risedronate versus no treatment in one trial (13 participants) and whole-body vibration versus a placebo device in the second (21 participants). Both studies reported improved bone mineral density with the active treatments, with no improvement in the control groups, but the abstracts did not compare treatment and control conditions. All children tolerated whole-body vibration treatment. No study provided information on adverse events. Two studies are ongoing: one investigating whole-body vibration, the other investigating zoledronic acid.Authors' conclusions: We know of no high-quality evidence from RCTs to guide use of treatments to prevent or treat corticosteroid-induced osteoporosis and reduce the risk of fragility fractures in children and adults with DMD; only limited results from two trials reported in abstracts were available. We await formal trial reports. Findings from two ongoing relevant studies and two trials, for which only abstracts are available, will be important in future updates of this review.
机译:背景:皮质类固醇激素治疗被认为是杜氏肌营养不良症(DMD)的“黄金标准”。然而,还已知诱发骨质疏松症并因此增加椎骨脆性骨折的风险。对DMD患者的良好护理需要预防这些不良反应。增加骨矿物质密度的治疗方法包括双膦酸盐,维生素D和钙补充剂,以及青春期延迟青春期的睾丸激素。目的:评估长期服用皮质类固醇激素对DMD儿童和成人的预防和治疗骨质疏松的干预措施的效果。评估这些干预措施对椎骨脆性骨折和长骨骨折的发生频率以及生活质量的影响;搜索方法:2016年9月12日,我们搜索了Cochrane神经肌肉专门注册机构,CENTRAL,MEDLINE,Embase和CINAHL Plus,以鉴定可能合格的试验。我们还搜索了《 Web of Science ISI会议录》(2001年至2016年9月)和三个临床试验注册中心,以识别未发表的研究和正在进行的试验。我们联系了纳入研究的通讯作者,以获取有关未发表研究或进行中研究的信息。选择标准:我们考虑将纳入任何涉及骨皮质激素干预的骨骼健康干预措施的随机对照试验(RCT)和准RCT纳入评估。确诊为DMD的儿童,青少年和成人引起的骨质疏松和脆性骨折。干预措施可能包括口服和静脉注射双膦酸盐,维生素D补充剂,钙补充剂,饮食中的钙,睾丸激素和负重活动。数据收集和分析:两位评价作者按照标准的Cochrane方法对报告进行了独立评估并选择了潜在的纳入研究。我们联系研究作者以获取更多信息,以澄清已发表的工作,未发表的研究和进行中的工作。主要结果:我们确定了18项潜在研究,其中两项目前仅作为摘要报告,符合本评价的纳入标准。信息不足,无法提供完整的结果或无法充分评估偏倚的风险。参与者是5到15岁患有DMD的儿童(可移动和非可移动)。一项试验中,干预措施为利塞膦酸盐治疗,无治疗(13名参与者),第二项试验为全身振动治疗与安慰剂治疗(21名参与者)。两项研究均表明,积极治疗可改善骨矿物质密度,对照组无改善,但摘要未比较治疗和对照条件。所有儿童都可以接受全身振动治疗。没有研究提供不良事件的信息。正在进行两项研究:一项研究全身振动,另一项研究唑来膦酸。作者的结论:我们从RCT尚无高质量的证据来指导预防或治疗皮质类固醇激素引起的骨质疏松症并降低其风险的方法。 DMD儿童和成人的脆性骨折;仅提供了摘要中报道的两项试验的有限结果。我们等待正式的审判报告。两项正在进行的相关研究和两项试验的结果(仅提供摘要)对于将来进行本综述很重要。

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