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首页> 外文期刊>Bone Reports >What is the relationship between bone turnover markers and skeletal-related events in patients with bone metastases from solid tumors and in patients with multiple myeloma? A systematic review and meta-regression analysis
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What is the relationship between bone turnover markers and skeletal-related events in patients with bone metastases from solid tumors and in patients with multiple myeloma? A systematic review and meta-regression analysis

机译:来自实体肿瘤的骨转移患者和多发性骨髓瘤患者的骨转移标记和骨骼相关事件之间的关系是什么?系统审查和元回归分析

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IntroductionAs a result of the negative impact of bone metastases on patient quality of life, it is important to identify patients at increased risk of skeletal-related events (SREs). Biochemical markers produced by osteoblasts and osteoclasts may provide an early indicator of treatment response to antiresorptive therapy. We aimed to explore the relationship between change in the urinary bone turnover marker cross-linked N-terminal telopeptide of type 1 collagen (uNTX) at the earliest time of steady state and risk of SREs.MethodsA comprehensive search of eight bibliographic databases and two trial registries was conducted (June 2017). We included randomized controlled trials of adults (≥18?years old) with bone metastases from solid tumors (including breast, lung, prostate) or bone lesions from multiple myeloma that compared denosumab or bisphosphonate(s) with each other or a placebo. Meta-analyses were used to evaluate the relationship between uNTX and SREs. The primary outcomes were based on uNTX at week 13 and SREs in those studies.ResultsSeventeen studies (12,130 patients) were included. The analysis results indicated a positive association between uNTX reduction, measured by the between-group difference of the natural logarithm of the ratio between uNTX at week 13 and baseline, and SRE risk reduction, measured by the natural logarithm of the hazard ratio (HR) for time to first SRE between the two groups (uNTX effect on SRE risk, defined as SRE HR increase corresponding to one unit smaller in the magnitude of uNTX reduction: 0.3560, 95% confidence interval 0.0249–0.6871;P?=?.0390, R2?=?0.7360). Results were similar for studies that reported change in uNTX from baseline to week 13 and to later than week 13. The limitation of this review is that it depends on how comprehensive study data were that could be included in the meta-regression.ConclusionsOur findings support a positive relationship between reduction of bone turnover markers at the earliest time of steady state and reduction in longer-term risk of SREs.
机译:引入导出骨转移对患者生活质量的负面影响,重要的是识别患者有关的骨骼相关事件(SRES)的风险增加。由成骨细胞和破骨细胞产生的生化标志物可以提供对抗反射治疗的治疗反应的早期指标。我们的目标是在最早的稳态时间和SRES的风险中探讨1型胶原(UNTX)的交联N-末端细胞胨交联N-末端细胞胨的变化与SRES的风险。方法综合搜索八个书目数据库和两项试验注册管理机构进行(2017年6月)。我们包括来自多种骨髓瘤的固体肿瘤(包括乳腺癌,肺,前列腺)或骨病变的骨转移的随机对照试验,所述骨髓瘤与彼此或安慰剂相比Denosumab或双膦酸盐的骨骼转移。 Meta分析用于评估UNTX和SRE之间的关系。主要结果是基于Untx,在第13周,并在那些研究中进行SRES.CESULSSEENEN研究(12,130名患者)。分析结果表明,在第13周的第13周和基线之间的自然对数的分组差异,通过危险比的自然对数(HR)测量的基线之间的基线之间的分组差异,通过危险比(HR)的自然对数来测量的阳性关联。在两组之间的第一次SRE(对SRE风险的UNTX影响,定义为SRE HR增加到一个单位,对应于UNTX的幅度较小:0.3560,95%置信区间0.0249-0.6871; p?= 0390, R2?=?0.7360)。结果类似于研究基线从基线报告到第13周和第13周的第13周的改变。本次审查的限制是它取决于全面的研究数据如何包含在元回归中.Conclusionsour调查结果支持在稳态稳定时间的最早时间减少骨周转标记的阳性关系,降低Sres的长期风险。

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