Bozaci Ayse Ergül, Er Esra, Ünal Aysel Tekmenuray, Taş İbrahim, Ayaz Ercan, Ozbek Mehmet Nuri, Durmaz Asude, Aykut Ayçe, Kose Melis
Diyarbakır Children's Hospital, Department of Pediatrics, Division of Pediatric Metabolism, Diyarbakir, Turkey.
Tepecik Research and Training Hospital, Department of Pediatrics, Division of Pediatric Metabolism, Izmir, Turkey.
Mol Genet Metab Rep. 2023 May 23;36:100979. doi: 10.1016/j.ymgmr.2023.100979. eCollection 2023 Sep.
Cerebral organic acid disorders are progressive neurometabolic diseases characterized by neurologic dysfunction. Glutaric aciduria type I (GA-I) and L-2-hydroxyglutaric aciduria (L2HGA) are the main cerebral organic acid disorders. They are both classified as, and it is suggested that these two disorders may share a common metabolic pathway. Current treatment strategies are based on levocarnitine, vitamin B2, and diet. Recent guidelines recommend a lysine-restricted diet up to six years of age, but there is no consensus for patients over the age of six. Vitamin B2 is exists in the blood as riboflavin and its cofactors, flavin mononucleotide and flavin adenine dinucleotide (FAD). FAD, the cofactor of L2HGD, accelerates the conversion of L-2-hydoxy glutarate to alpha-ketoglutarate. Levocarnitine stimulates the formation and excretion of derivatives of glutaric acid. Also, lysine-associated organic acidurias some results provide principal proof for the beneficial effects of riboflavin in GA-I. It has been previously reported that combination therapy with riboflavin and levocarnitine is effective for L2HGA as well as GA-I. Riboflavin and levocarnitine have been reported to improve not only clinical symptoms but also urinary 2-HGA levels. In our study, we aimed to evaluate the effect of the current treatment strategies and genotype on urinary metabolites and IQ scores in GA-I and L2HGA patients.
The presented retrospective multicenter study included patients followed up in Diyarbakir Children's Hospital and Izmir Katip Celebi University Faculty of Medicine, Division of Pediatric Metabolism. Between 2016 and 2021, we retrospectively evaluated 35 patients with confirmed diagnosis of GA-I and L-2HGA. We analyzed the clinical, biochemical, neuroradiological, molecular data and treatment of the patients. The follow-up period was every 2 months until 12 months old, every 3 months until 6 years of age, and every 6 months thereafter. Therapy monitoring was undertaken during follow-up visits that included evaluation of clinical parameters, laboratory parameters, and dietary consumption records. Denver II was applied in order to evaluate children aged 0-6 years in terms of development. Patients between 6 and 16 years of age were evaluated using the Wechsler Intelligence Scale for Children-Revised.
We identified 25 with GA-I and 10 with L2HGA. The most common clinical symptoms were developmental delay, intellectual disability, and movement disorders. Behavioural problems were more common in L2HGA than in GA-I patients. In the same family, there were patients with severe developmental delay despite early diagnosis and treatment and individuals with normal IQ scores. In our study group, we used diet (lysine restricted or protein controlled), levocarnitine and vitamin B2 for GA-I patients. The mean urinary glutaric acid levels were decreased with treatment in GA-I patients. Group I consisted of 14/25 patients receiving lysine restricted diet and levocarnitine, Group II (8/25) received protein-controlled diet and levocarnitine. Group III (3/25) patients whom had p.Pro248Leu (P248L) variant, received riboflavin in combination with protein-controlled diet and levocarnitine. When we evaluated according to the treatment groups, a significant decrease was observed in urinary glutaric acid levels in group I. But there were no significant difference in Group II and III. The patients with c.1018C > T variant in GCDH gene had higher pre-treatment urinary metabolites and significant reduction in urinary metabolites with treatment was detected. In L2HGA patients, we used levocarnitine and vitamin B2. In all L2HGA patients, there was a significant decrease in the mean urinary 2- hydoxy glutarate with treatment. However, there was no significant difference between the c.164G > A and c.1115delT variants. The mean pre- and post-treatment IQ scores of GA-I patients, no significant difference was observed. Relative neurologic improvement was seen in three L2HGA patients. We found two novel variants, including the c.221A > G (p.Tyr74Cys) in the GCDH gene and the c.738 + 5A > G splice variant in the L2HGDH gene.
Glutaric aciduria type I and L2HGA are the most common cerebral organic acidurias. Early and correct diagnosis is crucial. Poor prognosis based on metabolic crises and progressive deterioration still appears. In countries where newborn screening is not performed, a clinical suspicion index is required for cerebral organic aciduria. GA-I and L-2HGA are difficult to examine by medical evidence standards because of the small sample size, regional differences in newborn screening, and medical care limits. More clinical studies are needed to identify effective treatments. However, the significant decrease in urinary glutaric acid levels after treatment in patients on lysine-restricted diet raises the question of whether lysine-restricted diet should be continued after six years of age. We also reported our experience in order to contribute to the literature.
脑有机酸紊乱是一类以神经功能障碍为特征的进行性神经代谢疾病。I型戊二酸尿症(GA-I)和L-2-羟基戊二酸尿症(L2HGA)是主要的脑有机酸紊乱疾病。它们都被归类为,并且有人认为这两种疾病可能共享一条共同的代谢途径。目前的治疗策略基于左卡尼汀、维生素B2和饮食。最近的指南建议在6岁之前采用赖氨酸限制饮食,但对于6岁以上的患者尚无共识。维生素B2在血液中以核黄素及其辅因子黄素单核苷酸和黄素腺嘌呤二核苷酸(FAD)的形式存在。FAD是L2HGD的辅因子,可加速L-2-羟基戊二酸向α-酮戊二酸的转化。左卡尼汀刺激戊二酸衍生物的形成和排泄。此外,一些赖氨酸相关有机酸尿症的结果为核黄素对GA-I有益作用提供了主要证据。此前有报道称,核黄素和左卡尼汀联合治疗对L2HGA以及GA-I均有效。据报道,核黄素和左卡尼汀不仅能改善临床症状,还能降低尿中2-HGA水平。在我们的研究中,我们旨在评估当前治疗策略和基因型对GA-I和L2HGA患者尿代谢物和智商分数的影响。
本回顾性多中心研究纳入了在迪亚巴克尔儿童医院和伊兹密尔卡迪普·切莱比大学医学院儿科代谢科随访的患者。在2016年至2021年期间,我们回顾性评估了35例确诊为GA-I和L-2HGA的患者。我们分析了患者的临床、生化、神经放射学、分子数据及治疗情况。随访期为12个月龄前每2个月一次,6岁前每3个月一次,此后每6个月一次。在随访期间进行治疗监测,包括评估临床参数、实验室参数和饮食摄入记录。应用丹佛发育筛查测验第二版评估0至6岁儿童的发育情况。6至16岁的患者使用韦氏儿童智力量表修订版进行评估。
我们确定了25例GA-I患者和10例L2HGA患者。最常见的临床症状是发育迟缓、智力残疾和运动障碍。行为问题在L2HGA患者中比在GA-I患者中更常见。在同一家族中,尽管早期诊断和治疗,但仍有严重发育迟缓的患者以及智商分数正常的个体。在我们的研究组中,我们对GA-I患者使用饮食(赖氨酸限制或蛋白质控制)、左卡尼汀和维生素B2。GA-I患者治疗后尿戊二酸平均水平降低。第一组由14/25例接受赖氨酸限制饮食和左卡尼汀的患者组成,第二组(8/25)接受蛋白质控制饮食和左卡尼汀。第三组(3/25)具有p.Pro248Leu(P248L)变异的患者,接受核黄素联合蛋白质控制饮食和左卡尼汀。当我们根据治疗组进行评估时,第一组尿戊二酸水平显著降低。但第二组和第三组无显著差异。GCDH基因中c.1018C>T变异的患者治疗前尿代谢物水平较高,治疗后尿代谢物显著降低。在L2HGA患者中,我们使用左卡尼汀和维生素B2。所有L2HGA患者治疗后尿2-羟基戊二酸平均水平显著降低。然而,c.164G>A和c.1115delT变异之间无显著差异。GA-I患者治疗前后的平均智商分数无显著差异。3例L2HGA患者出现相对神经功能改善。我们发现了两个新变异,包括GCDH基因中的c.221A>G(p.Tyr74Cys)和L2HGDH基因中的c.738+5A>G剪接变异。
I型戊二酸尿症和L2HGA是最常见的脑有机酸尿症。早期正确诊断至关重要。基于代谢危机和进行性恶化的不良预后仍然存在。在未开展新生儿筛查的国家,对于脑有机酸尿症需要有临床怀疑指数。由于样本量小、新生儿筛查的地区差异和医疗保健限制,GA-I和L-2HGA难以按照医学证据标准进行研究。需要更多的临床研究来确定有效的治疗方法。然而,赖氨酸限制饮食患者治疗后尿戊二酸水平显著降低,这引发了6岁后是否应继续赖氨酸限制饮食的问题。我们也报告了我们的经验以丰富文献。
