Alfadhel Majid, Abadel Basma, Almaghthawi Hind, Umair Muhammad, Rahbeeni Zuhair, Faqeih Eissa, Almannai Mohammed, Alasmari Ali, Saleh Mohammed, Eyaid Wafaa, Alfares Ahmed, Al Mutairi Fuad
Genetics and Precision Medicine Department, King Abdullah Specialized Children Hospital, King Abdulaziz Medical City MNG-HA, Riyadh, Saudi Arabia.
Medical Genomics Research Department, King Abdullah International Medical Research Center (KAIMRC), King Saud Bin Abdulaziz University for Health Sciences, Ministry of National Guard Health Affairs (MNG-HA), Riyadh, Saudi Arabia.
Front Genet. 2022 May 13;13:880464. doi: 10.3389/fgene.2022.880464. eCollection 2022.
3-Hydroxy-3-methylglutaryl-coenzyme A lyase deficiency (HMG-CoA lyase) is a rare inborn error of leucine degradation and ketone body synthesis, caused by homozygous or compound heterozygous disease-causing variants in . To understand the natural history of this disease, we reviewed the biochemical, clinical, and molecular data of 62 patients from 54 different families with confirmed HMG-CoA lyase deficiency (HMGCLD) diagnosis from Saudi Arabia. The majority of the affected individuals were symptomatic. At initial diagnosis, 38 patients (61.29%) presented with hypoglycemia and 49 patients (79.03%) developed metabolic acidosis. In 27 patients (43.54%), the disorder manifested in the neonatal period, mostly within the first days of life, while 35 (56.45%) patients were diagnosed within the first year of life or beyond. All the patients were alive and developed long-term neurological complications during data collection, which may significantly influence their quality of life. Common neurological findings include seizures 17/62 (27.41%), hypotonic 3/62 (4.83%), speech delay 7/62 (11.29%), hyperactivity 4/62 (4.83%), developmental delay 6/62 (9.677%), learning disability 15/62 (24.14%), and ataxic gate 1/62 (1.612%). An MRI of the brain exhibited nonspecific periventricular and deep white matter hyperintense signal changes in 16 patients (25.80%) and cerebral atrophy was found in one (1/62; 1.612%) patient. We identified a founder variant [c.122G>A; p.(Arg41Gln)] in 48 affected individuals (77.41%) in the gene. This is the largest cohort of HMGCLD patients reported from Saudi Arabia, signifying this disorder as a likely life-threatening disease, with a high prevalence in the region. Our findings suggest that diagnosis at an early stage with careful dietary management may avoid metabolic crises.
3-羟基-3-甲基戊二酰辅酶A裂解酶缺乏症(HMG-CoA裂解酶缺乏症)是一种罕见的先天性亮氨酸降解和酮体合成障碍疾病,由纯合或复合杂合致病变体引起。为了解该疾病的自然病史,我们回顾了来自沙特阿拉伯54个不同家庭的62例确诊为HMG-CoA裂解酶缺乏症(HMGCLD)患者的生化、临床和分子数据。大多数受影响个体有症状。初诊时,38例患者(61.29%)出现低血糖,49例患者(79.03%)发生代谢性酸中毒。27例患者(43.54%)在新生儿期发病,大多在出生后的头几天,而35例患者(56.45%)在1岁以内或之后被诊断。在数据收集期间,所有患者均存活并出现了长期神经并发症,这可能会显著影响他们的生活质量。常见的神经学表现包括癫痫发作17/62(27.41%)、肌张力低下3/62(4.83%)、语言发育迟缓7/62(11.29%)、多动4/62(4.83%)、发育迟缓6/62(9.677%)、学习障碍15/62(24.14%)和共济失调步态1/62(1.612%)。16例患者(25.80%)的脑部MRI显示脑室周围和深部白质非特异性高信号改变,1例患者(1/62;1.612%)发现脑萎缩。我们在该基因的48例受影响个体(77.41%)中鉴定出一个奠基者变体[c.122G>A;p.(Arg41Gln)]。这是沙特阿拉伯报告的最大一组HMGCLD患者队列,表明这种疾病可能是一种危及生命的疾病,在该地区患病率很高。我们的研究结果表明,早期诊断并进行仔细的饮食管理可能避免代谢危机。
