Li Xue, Meng Xiangrui, Timofeeva Maria, Tzoulaki Ioanna, Tsilidis Konstantinos K, Ioannidis John PA, Campbell Harry, Theodoratou Evropi
Centre for Global Health Research, Usher Institute of Population Health Sciences and Informatics, University of Edinburgh, Edinburgh EH8 9AG, UK.
Colon Cancer Genetics Group, Medical Research Council Human Genetics Unit, Medical Research Council Institute of Genetics & Molecular Medicine, University of Edinburgh, Edinburgh, UK.
BMJ. 2017 Jun 7;357:j2376. doi: 10.1136/bmj.j2376.
To map the diverse health outcomes associated with serum uric acid (SUA) levels. Umbrella review. Medline, Embase, Cochrane Database of Systematic Reviews, and screening of citations and references. Systematic reviews and meta-analyses of observational studies that examined associations between SUA level and health outcomes, meta-analyses of randomised controlled trials that investigated health outcomes related to SUA lowering treatment, and Mendelian randomisation studies that explored the causal associations of SUA level with health outcomes. 57 articles reporting 15 systematic reviews and144 meta-analyses of observational studies (76 unique outcomes), 8 articles reporting 31 meta-analyses of randomised controlled trials (20 unique outcomes), and 36 articles reporting 107 Mendelian randomisation studies (56 unique outcomes) met the eligibility criteria. Across all three study types, 136 unique health outcomes were reported. 16 unique outcomes in meta-analyses of observational studies had P<10, 8 unique outcomes in meta-analyses of randomised controlled trials had P<0.001, and 4 unique outcomes in Mendelian randomisation studies had P<0.01. Large between study heterogeneity was common (80% and 45% in meta-analyses of observational studies and of randomised controlled trials, respectively). 42 (55%) meta-analyses of observational studies and 7 (35%) meta-analyses of randomised controlled trials showed evidence of small study effects or excess significance bias. No associations from meta-analyses of observational studies were classified as convincing; five associations were classified as highly suggestive (increased risk of heart failure, hypertension, impaired fasting glucose or diabetes, chronic kidney disease, coronary heart disease mortality with high SUA levels). Only one outcome from randomised controlled trials (decreased risk of nephrolithiasis recurrence with SUA lowering treatment) had P<0.001, a 95% prediction interval excluding the null, and no large heterogeneity or bias. Only one outcome from Mendelian randomisation studies (increased risk of gout with high SUA levels) presented convincing evidence. Hypertension and chronic kidney disease showed concordant evidence in meta-analyses of observational studies, and in some (but not all) meta-analyses of randomised controlled trials with respective intermediate or surrogate outcomes, but they were not statistically significant in Mendelian randomisation studies. Despite a few hundred systematic reviews, meta-analyses, and Mendelian randomisation studies exploring 136 unique health outcomes, convincing evidence of a clear role of SUA level only exists for gout and nephrolithiasis.
为明确与血清尿酸(SUA)水平相关的多种健康结局。伞状综述。检索Medline、Embase、Cochrane系统评价数据库,并筛选文献及参考文献。纳入观察性研究的系统评价和荟萃分析,这些研究考察了SUA水平与健康结局之间的关联;纳入随机对照试验的荟萃分析,这些试验研究了与降低SUA治疗相关的健康结局;纳入孟德尔随机化研究,这些研究探索了SUA水平与健康结局之间的因果关联。57篇文章报告了15项系统评价和144项观察性研究的荟萃分析(76个独特结局),8篇文章报告了31项随机对照试验的荟萃分析(20个独特结局),36篇文章报告了107项孟德尔随机化研究(56个独特结局)符合纳入标准。在所有三种研究类型中,共报告了136个独特的健康结局。观察性研究荟萃分析中的16个独特结局P<0.01,随机对照试验荟萃分析中的8个独特结局P<0.001,孟德尔随机化研究中的4个独特结局P<0.01。研究间的较大异质性很常见(观察性研究和随机对照试验的荟萃分析中分别为80%和45%)。42项(55%)观察性研究的荟萃分析和7项(35%)随机对照试验的荟萃分析显示存在小研究效应或过度显著性偏差的证据。观察性研究荟萃分析中的关联均未被归类为有说服力的;五项关联被归类为高度提示性(高SUA水平会增加心力衰竭、高血压、空腹血糖受损或糖尿病、慢性肾脏病、冠心病死亡的风险)。随机对照试验中只有一个结局(降低SUA治疗后肾结石复发的风险)P<0.001,95%预测区间不包括无效值,且无较大异质性或偏差。孟德尔随机化研究中只有一个结局(高SUA水平会增加痛风风险)提供了有说服力的证据。高血压和慢性肾脏病在观察性研究的荟萃分析以及一些(但并非全部)有各自中间或替代结局的随机对照试验荟萃分析中显示出一致的证据,但在孟德尔随机化研究中无统计学意义。尽管有数百项系统评价、荟萃分析和孟德尔随机化研究探索了136个独特的健康结局,但只有痛风和肾结石有明确证据表明SUA水平发挥了明确作用。
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