基于孟德尔随机化的炎症性肠病与骨密度相关性研究。
Mendelian randomization study of inflammatory bowel disease and bone mineral density.
机构信息
Department of Orthopaedics, Union Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, 430022, China.
Department of Otorhinolaryngology, The Third Hospital of Wuhan City, Wuhan, 430070, China.
出版信息
BMC Med. 2020 Nov 10;18(1):312. doi: 10.1186/s12916-020-01778-5.
BACKGROUND
Recently, the association between inflammatory bowel disease (including ulcerative colitis and Crohn's disease) and BMD has attracted great interest in the research community. However, the results of the published epidemiological observational studies on the relationship between inflammatory bowel disease and BMD are still inconclusive. Here, we performed a two-sample Mendelian randomization analysis to investigate the causal link between inflammatory bowel disease and level of BMD using publically available GWAS summary statistics.
METHODS
A series of quality control steps were taken in our analysis to select eligible instrumental SNPs which were strongly associated with exposure. To make the conclusions more robust and reliable, we utilized several robust analytical methods (inverse-variance weighting, MR-PRESSO method, mode-based estimate method, weighted median, MR-Egger regression, and MR.RAPS method) that are based on different assumptions of two-sample MR analysis. The MR-Egger intercept test, Cochran's Q test, and "leave-one-out" sensitivity analysis were performed to evaluate the horizontal pleiotropy, heterogeneities, and stability of these genetic variants on BMD. Outlier variants identified by the MR-PRESSO outlier test were removed step-by-step to reduce heterogeneity and the effect of horizontal pleiotropy.
RESULTS
Our two-sample Mendelian randomization analysis with two groups of exposure GWAS summary statistics and four groups of outcome GWAS summary statistics suggested a definitively causal effect of genetically predicted ulcerative colitis on TB-BMD and FA-BMD but not on FN-BMD or LS-BMD (after Bonferroni correction), and we merely determined a causal effect of Crohn's disease on FN-BMD but not on the others, which was somewhat inconsistent with many published observational researches. The causal effect of inflammatory bowel disease on TB-BMD was significant and robust but not on FA-BMD, FN-BMD, and LS-BMD, which might result from the cumulative effect of ulcerative colitis and Crohn's disease on BMDs.
CONCLUSIONS
Our Mendelian randomization analysis supported the causal effect of ulcerative colitis on TB-BMD and FA-BMD. As to Crohn's disease, only the definitively causal effect of it on decreased FN-BMD was observed. Updated MR analysis is warranted to confirm our findings when a more advanced method to get less biased estimates and better precision or GWAS summary data with more ulcerative colitis and Crohn's disease patients was available.
背景
最近,炎症性肠病(包括溃疡性结肠炎和克罗恩病)与 BMD 的关联引起了研究界的极大兴趣。然而,已发表的关于炎症性肠病与 BMD 之间关系的流行病学观察研究结果仍不确定。在这里,我们使用公开的 GWAS 汇总统计数据进行了两样本 Mendelian 随机化分析,以研究炎症性肠病与 BMD 水平之间的因果关系。
方法
在我们的分析中进行了一系列质量控制步骤,以选择与暴露强烈相关的合格工具性 SNP。为了使结论更加稳健可靠,我们利用了几种基于两样本 MR 分析不同假设的稳健分析方法(逆方差加权、MR-PRESSO 方法、基于模式的估计方法、加权中位数、MR-Egger 回归和 MR.RAPS 方法)。进行了 MR-Egger 截距检验、Cochran's Q 检验和“逐一剔除”敏感性分析,以评估这些遗传变异对 BMD 的水平遗传异质性和稳定性。通过 MR-PRESSO 异常值检验识别出的异常值变体被逐步剔除,以减少异质性和水平遗传异质性的影响。
结果
我们的两样本 Mendelian 随机化分析使用两组暴露 GWAS 汇总统计数据和四组结局 GWAS 汇总统计数据,表明遗传预测的溃疡性结肠炎对 TB-BMD 和 FA-BMD 具有明确的因果作用,但对 FN-BMD 或 LS-BMD 没有(经过 Bonferroni 校正),并且我们仅确定了克罗恩病对 FN-BMD 的因果作用,但对其他作用没有,这与许多已发表的观察性研究有些不一致。炎症性肠病对 TB-BMD 的因果作用是显著且稳健的,但对 FA-BMD、FN-BMD 和 LS-BMD 则不然,这可能是溃疡性结肠炎和克罗恩病对 BMDs 的累积作用所致。
结论
我们的 Mendelian 随机化分析支持溃疡性结肠炎对 TB-BMD 和 FA-BMD 的因果作用。至于克罗恩病,仅观察到其对 FN-BMD 降低的明确因果作用。当获得更先进的方法来获得更无偏估计和更好的精度或具有更多溃疡性结肠炎和克罗恩病患者的 GWAS 汇总数据时,需要进行更新的 MR 分析来证实我们的发现。
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