与 2,4-二烯酰基辅酶 A 还原酶 1 缺乏相关的脂肪变性肝病。
Steatotic liver disease associated with 2,4-dienoyl-CoA reductase 1 deficiency.
机构信息
Department of General Paediatrics, Medical University of Graz, 8010, Graz, Austria.
Diagnostic and Research Institute of Pathology, Medical University of Graz, 8010, Graz, Austria.
出版信息
Int J Obes (Lond). 2024 Dec;48(12):1818-1821. doi: 10.1038/s41366-024-01634-z. Epub 2024 Sep 14.
BACKGROUND
Metabolic dysfunction-associated steatotic liver disease (MASLD) is considered multifactorial with a number of predisposing gene polymorphisms known.
METHODS
The occurrence of MASLD in 7 and 10 year old siblings, one without classical risk factors and one with type 2 diabetes suggested a monogenic etiology and prompted next-generation sequencing. Exome sequencing was performed in the proband, both parents and both siblings. The impact of a likely disease-causing DNA variant was assessed on the transcript and protein level.
RESULTS
Two siblings have hepatomegaly, elevated serum transaminase activity, and steatosis and harbor a homozygous DECR1 splice-site variant, c.330+3A>T. The variant caused DECR1 transcript decay. Immunostaining demonstrated lack of DECR1 in patient liver.
CONCLUSIONS
These patients may represent the first individuals with DECR1 deficiency, then defining within MASLD an autosomal-recessive entity, well corresponding to the reported steatotic liver disease in Decr1 knockout mice. DECR1 may need to be considered in the genetic work-up of MASLD.
背景
代谢功能障碍相关脂肪性肝病 (MASLD) 被认为是多因素的,有许多已知的易患基因多态性。
方法
7 岁和 10 岁的同卵双胞胎兄妹均患有 MASLD,其中一位无经典危险因素,另一位患有 2 型糖尿病,提示其病因具有单基因性,并促使进行下一代测序。对先证者、父母双方和两个兄弟姐妹进行了外显子组测序。评估了一种可能的致病 DNA 变异对转录本和蛋白质水平的影响。
结果
两个兄弟姐妹均有肝肿大、血清转氨酶活性升高和脂肪变性,并携带 DECR1 剪接位点的纯合变异 c.330+3A>T。该变异导致 DECR1 转录本降解。免疫染色显示患者肝脏中 DECR1 缺失。
结论
这些患者可能是 DECR1 缺乏症的首批个体,然后在 MASLD 中定义为常染色体隐性实体,与 Decr1 基因敲除小鼠报告的脂肪性肝病非常吻合。在 MASLD 的遗传分析中可能需要考虑 DECR1。
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