马来西亚儿童高同型半胱氨酸血症的临床、生化、分子特征和临床结果

IF 2.5 3区医学 Q2 MEDICAL LABORATORY TECHNOLOGY

Clinical biochemistry Pub Date : 2024-09-23 DOI:10.1016/j.clinbiochem.2024.110828

Anasufiza Habib , Hamizah Idrus , Nur Aisyah Abdul Malik , Ainna Mohd Nor , Sofwatul Muktaroh Nasohah , Lip Hen Moey , Lua Seok Hian , Ngu Lock Hock , Nor Azimah Abdul Azize

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引用次数: 0

摘要

背景高同型半胱氨酸血症可由蛋氨酸、叶酸和维生素 B12 的复杂相互作用的各种异常引起。众所周知，高同型半胱氨酸血症是心血管风险因素之一。本研究旨在回顾马来西亚被诊断为严重高同型半胱氨酸血症的儿科患者的临床表现、潜在原因和临床结果。2010年至2022年期间，对96721名患者进行了选择性高风险筛查，从中确定了患有严重高同型半胱氨酸血症的儿科患者。研究的纳入标准是患有严重高同型半胱氨酸血症（40 µmol/L）的儿科患者。胱硫醚β-合成酶缺乏症（CBS）患者的平均同型半胱氨酸总量（tHcy）和蛋氨酸含量分别为 269 µmol/L 和 499 µmol/L，再甲基化缺陷患者的平均同型半胱氨酸总量（tHcy）和蛋氨酸含量分别为 127 µmol/L 和 29 µmol/L，先天性 B12 缺乏症患者的平均同型半胱氨酸总量（tHcy）和蛋氨酸含量分别为 390 µmol/L 和 4 µmol/L。我们发现，c.609G>A 是 MMACHC 基因最常见的突变，而 CBS（c.402del、c.1333C>T 和 c.1031T>G）和 MTHFR 基因（c.266T>A 和 c.1249del）可能存在新的突变。进一步的亚分类显示，5/16 的患者患有 CBS（31%），9/16 的患者患有再甲基化缺陷（56%），2/16 的患者患有先天性 B12 缺乏症（13%）。所有患者都接受了标准治疗和主要生物标志物的定期监测。确诊时的平均年龄为 9.2 岁（CBS）和 1.2 岁（再甲基化缺陷）。先天性 B12 缺乏症患者有轻微的发育迟缓，再甲基化缺陷患者有轻度至中度的学习障碍，CBS 患者有不同程度的智力障碍、发育迟缓、眼科异常，并在青春期/成年早期出现血栓。建议对马来西亚儿童进行高同型半胱氨酸血症筛查，以便尽早治疗并改善临床结果。

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Clinical, biochemical, molecular characteristics and clinical outcome of hyperhomocysteinemia in Malaysian children

Background

Hyperhomocysteinemia can be due to various abnormalities of the complex interaction of methionine, folate and vitamin B12. It has been known to be a cardiovascular risk factor. This study aims to review the clinical presentation, underlying causes and clinical outcome in paediatric patients diagnosed with significant hyperhomocysteinemia in Malaysia.

Design and methods

Data were obtained from the medical records and the laboratory information system. Paediatric patients with significant hyperhomocysteinemia were identified from a selective high-risk screening of 96,721 patients, performed between 2010 and 2022. Inclusion criteria for the study were paediatric patients with significant hyperhomocysteinemia (>40 µmol/L).

Results

Sixteen patients were identified. The average total homocysteine (tHcy) and methionine were 269 µmol/L and 499 µmol/L in cystathionine β-synthase deficiency (CBS), 127 µmol/L and 29 µmol/L in patients with remethylation defects and 390 µmol/L and 4 µmol/L in congenital B12 deficiency. We found c.609G>A as the most prevalent mutation in MMACHC gene and possible novel mutations for CBS (c.402del, c.1333C>T and c.1031T>G) and MTHFR genes (c.266T>A and c.1249del). Further subclassification revealed CBS was 5/16 patients (31 %), remethylation defects was 9/16 (56 %) and congenital B12 deficiency was 2/16 (13 %). All patients received standard treatment and regular monitoring of the main biomarkers. The average age at the time of diagnosis were 9.2 years (CBS) and 1.2 years (remethylation defects). Congenital B12 deficiency had slight delay in milestones, remethylation defects had mild to moderate learning disabilities, CBS had variable degree of intellectual disability, delayed milestones, ophthalmological abnormalities, and thrombosis at an early adolescent/adulthood.

Conclusions

The majority of significant hyperhomocysteinemia in Malaysian children was due to remethylation defects. Screening for hyperhomocysteinemia in Malaysian children is recommended for earlier treatment and improved clinical outcome.

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来源期刊

Clinical biochemistry 医学-医学实验技术

CiteScore

5.10

自引率

0.00%

发文量

151

审稿时长

25 days

期刊介绍： Clinical Biochemistry publishes articles relating to clinical chemistry, molecular biology and genetics, therapeutic drug monitoring and toxicology, laboratory immunology and laboratory medicine in general, with the focus on analytical and clinical investigation of laboratory tests in humans used for diagnosis, prognosis, treatment and therapy, and monitoring of disease.