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Potential causal role of L-glutamine in sickle cell disease painful crises: A Mendelian randomization analysis

机译:L-谷氨酰胺在镰状细胞疾病痛苦危机中的潜在因果作用:孟德尔随机化分析

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In a recent clinical trial, the metabolite L-glutamine was shown to reduce painful crises in sickle cell disease (SCD) patients. To support this observation and identify other metabolites implicated in SCD clinical heterogeneity, we profiled 129 metabolites in the plasma of 705 SCD patients. We tested correlations between metabolite levels and six SCD-related complications (painful crises, cholecystectomy, retinopathy, leg ulcer, priapism, aseptic necrosis) or estimated glomerular filtration rate (eGFR), and used Mendelian randomization (MR) to assess causality. We found a potential causal relationship between L-glutamine levels and painful crises (N = 1278, odds ratio (OR) [95% confidence interval] = 0.68 [0.52-0.89], P = 0.0048). In two smaller SCD cohorts (N = 299 and 406), the protective effect of L-glutamine was observed (OR = 0.82 [0.50-1.34]), although the MR result was not significant (P = 0.44). We identified 66 significant correlations between the levels of other metabolites and SCD-related complications or eGFR. We tested these correlations for causality using MR analyses and found no significant causal relationship. The baseline levels of quinolinic acid were associated with prospectively ascertained survival in SCD patients, and this effect was dependent on eGFR. Metabolomics provide a promising approach to prioritize small molecules that may serve as biomarkers or drug targets in SCD.
机译:在最近的临床试验中,显示了代谢物L-谷氨酰胺,以减少镰状细胞疾病(SCD)患者的痛苦危机。为了支持这种观察结果并鉴定涉及SCD临床异质性的其他代谢物,我们在705例SCD患者的血浆中分析了129个代谢物。我们测试了代谢物水平与六种与SCD相关的并发症(痛苦的危机,胆囊切除术,视网膜病变,腿部溃疡,治疗,无菌坏死)或估计肾小球过滤率(EGFR)之间的相关性,以及使用孟德利安随机化(MR)来评估因果关系。我们发现L-谷氨酰胺水平和疼痛危机之间的潜在因果关系(n = 1278,差距比(或)[95%置信区间] = 0.68 [0.52-0.89],p = 0.0048)。在两个较小的SCD队列(n = 299和406)中,观察到L-谷氨酰胺的保护作用(或= 0.82 [0.50-1.34]),但MR结果不显着(p = 0.44)。我们确定了其他代谢物和SCD相关并发症或EGFR水平之间的66个显着相关性。我们使用MR分析测试了这些因果关系的相关性,发现没有显着的因果关系。喹啉酸的基线水平与SCD患者的前瞻性上确定的存活相关,这种效果取决于EGFR。代谢组科提供了一种有希望的方法,优先考虑可以作为SCD中的生物标志物或药物靶标的小分子。

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