Williams Monika, Menkovic Iskren, Reitnauer Pamela, Gilbert Eileen, Koeberl Dwight, Young Sarah P, Stiles Ashlee R
Department of Pediatrics, Division of Pediatric Genetics and Metabolism, UNC, Chapel Hill, NC, USA.
Biochemical Genetics Laboratory, Duke University Health System, Durham, NC, USA.
Mol Genet Metab Rep. 2024 Feb 1;38:101062. doi: 10.1016/j.ymgmr.2024.101062. eCollection 2024 Mar.
Mitochondrial 3-hydroxy-3-methylglutaryl-CoA (HMG-CoA) synthase (mHS) deficiency is an autosomal recessive disorder of ketone body synthesis caused by biallelic pathogenic variants in . Clinical symptoms are precipitated by prolonged fasting and/or intercurrent illness with onset before the first year of life. Clinically, patients may present with hypo-/ non-ketotic hypoglycemia, metabolic acidosis, hyperammonemia, lethargy, hepatomegaly, and encephalopathy. During periods of decompensation, elevations of 4-hydroxy-6-methyl-2-pyrone (4-HMP), several hydroxylated hexanoic and hexenoic acid species, and medium-chain dicarboxylic acids in the absence of significant ketonuria may be observed in the urine organic acid profile. Abnormalities may also be observed in plasma which includes elevated acetylcarnitine (C2) and 3-hydroxybutyryl/3-hydroxyisobutyryl (C4-OH) carnitine. We report a patient who presented to the ED at 13 months of age with an undetectable point-of-care blood glucose level. Continuous infusion of dextrose-containing intravenous (IV) fluids were required to correct the hypoglycemia and routine chemistries were notable for an anion gap metabolic acidosis, transaminasemia, and elevated creatine kinase and lactate dehydrogenase. Urine and blood ketones were undetectable. Qualitative assessment of urine organic acids collected ∼46 and ∼ 99 h post-admission were significant for mild elevations of 4-HMP and hydroxy-hexanoic and hydroxy-hexenoic acid species with a notable absence of ketones. Previously, biochemical abnormalities in urine have been shown to normalize in as few as 27 h after treatment giving providers a narrow window with which to obtain a critical sample. Direct communication of laboratory findings to the ordering provider guided the molecular testing and assisted in results interpretation to confirm the molecular diagnosis. Our case emphasizes the importance of collecting samples for biochemical analysis even if the critical period has been missed and acute metabolic decompensation seems to be resolved, as residual abnormalities observed in our patient greatly narrowed the differential diagnosis.
线粒体3-羟基-3-甲基戊二酰辅酶A(HMG-CoA)合酶(mHS)缺乏症是一种常染色体隐性酮体合成障碍疾病,由 中的双等位基因致病变异引起。临床症状在出生后第一年内因长期禁食和/或并发疾病而引发。临床上,患者可能出现低酮血症/非酮血症性低血糖、代谢性酸中毒、高氨血症、嗜睡、肝肿大和脑病。在失代偿期,尿液有机酸谱中可观察到4-羟基-6-甲基-2-吡喃酮(4-HMP)、几种羟基己酸和己烯酸以及中链二羧酸升高,而尿酮体无明显升高。血浆中也可能观察到异常,包括乙酰肉碱(C2)和3-羟基丁酰/3-羟基异丁酰(C4-OH)肉碱升高。我们报告了一名13个月大的患者,其即时护理血糖水平检测不到,因低血糖被送往急诊科。需要持续输注含葡萄糖的静脉输液来纠正低血糖,常规化学检查显示存在阴离子间隙代谢性酸中毒、转氨酶升高以及肌酸激酶和乳酸脱氢酶升高。尿液和血液中的酮体检测不到。入院后约46小时和99小时收集的尿液有机酸定性评估显示,4-HMP以及羟基己酸和羟基己烯酸轻度升高,且明显无酮体。此前研究表明,治疗后尿液中的生化异常在短短27小时内即可恢复正常,这给医护人员获取关键样本的时间窗口很窄。实验室检查结果直接与开单医生沟通,指导了分子检测并协助结果解读以确认分子诊断。我们的病例强调了即使错过了关键时期且急性代谢失代偿似乎已得到解决,仍需采集样本进行生化分析的重要性,因为我们患者中观察到的残留异常极大地缩小了鉴别诊断范围。
