Sood Manish M, Murphy Malia S Q, Hawken Steven, Wong Coralie A, Potter Beth K, Burns Kevin D, Tsampalieros Anne, Atkinson Katherine M, Chakraborty Pranesh, Wilson Kumanan
The Ottawa Hospital Research Institute, Ottawa, Ontario, Canada.
Institute for Clinical Evaluative Sciences, Ottawa, Ontario, Canada.
Kidney Int Rep. 2018 Feb 10;3(3):691-700. doi: 10.1016/j.ekir.2018.02.001. eCollection 2018 May.
Metabolomics offers considerable promise in early disease detection. We set out to test the hypothesis that routine newborn metabolic profiles at birth, obtained through screening for inborn errors of metabolism, would be associated with kidney disease and add incremental information to known clinical risk factors.
We conducted a population-level cohort study in Ontario, Canada, using metabolic profiles from 1,288,905 newborns from 2006 to 2015. The primary outcome was chronic kidney disease (CKD) or dialysis. Individual metabolites and their ratio combinations were examined by logistic regression after adjustment for established risk factors for kidney disease and incremental risk prediction measured.
CKD occurred in 2086 (0.16%, median time 612 days) and dialysis in 641 (0.05%, median time 99 days) infants and children. Individual metabolites consisted of amino acids, acylcarnitines, markers of fatty acid oxidation, and others. Base models incorporating clinical risk factors only provided c-statistics of 0.61 for CKD and 0.70 for dialysis. The addition of identified metabolites to risk prediciton models resulted in significant incremental improvement in the performance of both models (CKD model: c-statistic 0.66 NRI 0.36 IDI 0.04, dialysis model: c-statistic 0.77 NRI 0.57 IDI 0.09). This was consistent after internal validation using bootstrapping and a sensitivity analysis excluding outcomes within the first 30 days.
Routinely collected screening metabolites at birth are associated with CKD and the need for dialytic therapies in infants and children, and add incremental information to traditional clinical risk factors.
代谢组学在疾病早期检测方面前景广阔。我们旨在验证这一假设,即通过筛查先天性代谢缺陷获得的新生儿出生时的常规代谢谱,将与肾脏疾病相关,并为已知的临床风险因素增加额外信息。
我们在加拿大安大略省进行了一项基于人群的队列研究,使用了2006年至2015年期间1,288,905名新生儿的代谢谱。主要结局是慢性肾脏病(CKD)或透析。在对既定的肾脏疾病风险因素进行调整并测量增量风险预测后,通过逻辑回归分析个体代谢物及其比值组合。
2086名婴儿和儿童发生了CKD(0.16%,中位时间612天),641名需要透析(0.05%,中位时间99天)。个体代谢物包括氨基酸、酰基肉碱、脂肪酸氧化标志物等。仅纳入临床风险因素的基础模型对CKD的c统计量为0.61,对透析的c统计量为0.70。将识别出的代谢物添加到风险预测模型中,两个模型的性能均有显著的增量改善(CKD模型:c统计量0.66,NRI 0.36,IDI 0.04;透析模型:c统计量0.77,NRI 0.57,IDI 0.09)。在使用自举法进行内部验证以及排除前30天内的结局进行敏感性分析后,结果一致。
出生时常规收集的筛查代谢物与婴儿和儿童的CKD及透析需求相关,并为传统临床风险因素增加了额外信息。
