37 例单纯性甲基丙二酸血症土耳其患者的临床和分子学发现。
Clinical and molecular findings in 37 Turkish patients with isolated methylmalonic acidemia.
机构信息
Department of Pediatric Metabolism, University of Mersin, Faculty of Medicine, Mersin, Turkey
Genetics and Genomics Medicine Department, Institute of Child Health, University College London, London, UK
出版信息
Turk J Med Sci. 2021 Jun 28;51(3):1220-1228. doi: 10.3906/sag-2001-72.
BACKGROUND/AIM: Isolated methylmalonic acidemia (MMA) is caused by complete or partial deficiency of the enzyme methylmalonyl- CoA mutase (mut0 or mut– enzymatic subtype), a defect of its cofactor adenosyl-cobalamin (cblA, cblB, or cblD-MMA), or deficiency of the enzyme methylmalonyl-CoA epimerase. While onset of the disease ranges from the neonatal period to adulthood, most cases present with lethargy, vomiting and ketoacidosis in the early infancy. Major secondary complications are; growth failure, developmental delay, interstitial nephritis with progressive renal failure, basal ganglia injury and cardiomyopathy. We aimed to demonstrate clinical and molecular findings based on long-term follow up in our patient cohort.
MATERIALS AND METHODS
The study includes 37 Turkish patients with isolated MMA who were followed up for long term complications 1 to 14 years. All patients were followed up regularly with clinical, biochemical and dietary monitoring to determine long term complications. Next Generation Sequencing technique was used for mutation screening in five disease-causing genes including; MUT, MMAA, MMAB, MMADHC, MCEE genes. Mutation screening identified 30 different types of mutations.
RESULTS
While 28 of these mutations were previously reported, one novel MMAA mutation p.H382Pfs*24 (c.1145delA) and one novel MUT mutation IVS3+1G>T(c.752+1G>T) has been reported. The most common clinical complications were growth retardation, renal involvement, mental motor retardation and developmental delay. Furthermore, one of our patients developed cardiomyopathy, another one died because of hepatic failure and one presented with lactic acidosis after linezolid exposure.
CONCLUSION
We have detected two novel mutations, including one splice-site mutation in the MUT gene and one frame shift mutation in the MMAA gene in 37 Turkish patients. We confirm the genotype-phenotype correlation in the study population according to the long-term complications.
背景/目的:孤立性甲基丙二酸血症(MMA)是由甲基丙二酰辅酶 A 变位酶(mut0 或 mut–酶亚型)完全或部分缺乏、其辅酶腺苷钴胺素(cblA、cblB 或 cblD-MMA)缺陷或甲基丙二酰辅酶 A 差向异构酶缺乏引起的。虽然疾病的发病时间从新生儿期到成年期不等,但大多数情况下,婴儿早期会出现嗜睡、呕吐和酮症酸中毒。主要的继发性并发症是:生长发育迟缓、发育迟缓、间质性肾炎伴进行性肾功能衰竭、基底节损伤和心肌病。我们旨在根据我们的患者队列的长期随访结果展示临床和分子发现。
材料和方法
该研究包括 37 名接受长期并发症随访的土耳其孤立性 MMA 患者,随访时间为 1 至 14 年。所有患者均定期进行临床、生化和饮食监测,以确定长期并发症。下一代测序技术用于包括 MUT、MMAA、MMAB、MMADHC 和 MCEE 基因在内的五个致病基因的突变筛查。突变筛查确定了 30 种不同类型的突变。
结果
其中 28 种突变是先前报道过的,一种新的 MMAA 突变 p.H382Pfs*24(c.1145delA)和一种新的 MUT 突变 IVS3+1G>T(c.752+1G>T)已被报道。最常见的临床并发症是生长迟缓、肾脏受累、精神运动发育迟缓和发育迟缓。此外,我们的一名患者发生了心肌病,另一名患者因肝功能衰竭死亡,一名患者在接触利奈唑胺后出现乳酸酸中毒。
结论
我们在 37 名土耳其患者中检测到两种新的突变,包括 MUT 基因中的一个剪接位点突变和 MMAA 基因中的一个移码突变。我们根据长期并发症在研究人群中证实了基因型-表型相关性。
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