Clinical Biochemistry Unit, Pathology Department, College of Medicine, King Saud University, Riyadh 11461, Saudi Arabia.
Metabolomics Section, Department of Clinical Genomics, Center for Genomics Medicine, King Faisal Specialist Hospital and Research Centre (KFSHRC), Riyadh 11211, KSA, Saudi Arabia.
Clin Chim Acta. 2024 Apr 15;557:117861. doi: 10.1016/j.cca.2024.117861. Epub 2024 Mar 13.
Glutaric aciduria type-1 (GA-1) is a rare metabolic disorder due to glutaryl coenzyme A dehydrogenase deficiency, causing elevated levels of glutaryl-CoA and its derivatives. GA-1 exhibits symptoms like macrocephaly, developmental delays, and movement disorders. Timely diagnosis through genetic testing and newborn screening is crucial. However, in some cases, transiently elevated level of glutarylcarnitine (C5DC) challenges accurate diagnosis, highlighting the need for alternative diagnostic methods, like mass spectrometry-based untargeted metabolomics, to identify additional biomarkers for distinguishing falsely suspected GA-1 from healthy newborns.
DBS samples from falsely suspected GA-1 newborns (n = 47) and matched control were collected through the NBS program. Untargeted metabolomics using liquid chromatography-high-resolution mass spectrometry (LC-HRMS) was performed to enable biomarker and pathway investigations for significantly altered metabolites.
582 and 546 were up- and down-regulated metabolites in transient GA-1. 155 endogenous metabolites displayed significant variations compared to the control group. Furthermore, our data identified novel altered metabolic biomarkers, such as N-palmitoylcysteine, heptacarboxyporphyrin, 3-hydroxylinoleoylcarnitine, and monoacylglyceride (MG) (0:0/20:1/0:0), along with perturbed metabolic pathways like sphingolipid and thiamine metabolism associated with the transient elevated C5DC levels in DBS samples.
A distinct metabolic pattern linked to the transient C5DC elevation in newborns was reported to enhance the prediction of the falsely positive cases, which could help avoiding unnecessary medical treatments and minimizing the financial burdens in the health sector.
1 型戊二酸血症(GA-1)是一种罕见的代谢紊乱疾病,由于戊二酰辅酶 A 脱氢酶缺乏,导致戊二酰辅酶 A 及其衍生物水平升高。GA-1 表现为大头畸形、发育迟缓、运动障碍等症状。通过基因检测和新生儿筛查及时诊断至关重要。然而,在某些情况下,一过性的戊二酰肉碱(C5DC)水平升高会挑战准确诊断,这凸显了需要替代的诊断方法,如基于质谱的非靶向代谢组学,以识别其他生物标志物,从而将疑似 GA-1 的病例与健康新生儿区分开来。
通过新生儿筛查计划收集疑似 GA-1 的新生儿(n=47)和匹配对照的 DBS 样本。采用液相色谱-高分辨率质谱(LC-HRMS)进行非靶向代谢组学分析,以研究显著改变的代谢物中的生物标志物和途径。
一过性 GA-1 中 582 个和 546 个代谢物上调和下调。与对照组相比,155 种内源性代谢物显示出显著的变化。此外,我们的数据还确定了新的改变的代谢生物标志物,如 N-棕榈酰半胱氨酸、七羧基卟啉、3-羟基亚油酸肉碱和单酰基甘油(MG)(0:0/20:1/0:0),以及与 DBS 样本中 C5DC 水平一过性升高相关的代谢途径,如鞘脂和硫胺素代谢的改变。
报告了与新生儿 C5DC 水平一过性升高相关的独特代谢模式,以增强对假阳性病例的预测,从而有助于避免不必要的医疗治疗并减轻卫生部门的经济负担。
