在一项前瞻性队列研究中,对非酒精性脂肪性肝病(NAFLD)瘦型个体的基因组分析确定了单基因疾病。
Genomic analysis of lean individuals with NAFLD identifies monogenic disorders in a prospective cohort study.
作者信息
Zheng Melanie, Huang Daniel Q, Konkwo Chigoziri, Agrawal Saaket, Khera Amit V, Loomba Rohit, Vilarinho Sílvia, Ajmera Veeral
机构信息
Departments of Internal Medicine, Section of Digestive Diseases, and of Pathology, Yale School of Medicine, New Haven, CT, USA.
NAFLD Research Center, Division of Gastroenterology, University of California at San Diego, La Jolla, CA, USA.
出版信息
JHEP Rep. 2023 Feb 2;5(4):100692. doi: 10.1016/j.jhepr.2023.100692. eCollection 2023 Apr.
BACKGROUND & AIMS: Lean patients with non-alcoholic fatty liver disease (NAFLD) represent 10-20% of the affected population and may have heterogeneous drivers of disease. We have recently proposed the evaluation of patients with lean NAFLD without visceral adiposity for rare monogenic drivers of disease. Here, we aimed to validate this framework in a well-characterised cohort of patients with biopsy-proven NAFLD by performing whole exome sequencing.
METHODS
This prospective study included 124 patients with biopsy-proven NAFLD and paired liver biopsies who underwent standardised research visits including advanced magnetic resonance imaging (MRI) assessment of liver fat and stiffness.
RESULTS
Six patients with lean NAFLD were identified and underwent whole exome sequencing. Two lean patients (33%) were identified to have monogenic disorders. The lean patients with monogenic disorders had similar age, and anthropometric and MRI characteristics to lean patients without a monogenic disorder. Patient 1 harbours a rare homozygous pathogenic mutation in (aldolase B) and was diagnosed with hereditary fructose intolerance. Patient 2 harbours a rare heterozygous mutation in apolipoprotein B (). The pathogenicity of this variant (p.Val1856CysfsTer2) was further validated in the UK Biobank and associated with lower circulating APOB levels (beta = -0.51 g/L, 95% CI -0.65 to -0.36 g/L, = 1.4 × 10) and higher liver fat on MRI (beta = +10.4%, 95% CI 4.3-16.5%, = 8.8 × 10). Hence, patient 2 was diagnosed with heterozygous familial hypobetalipoproteinaemia.
CONCLUSIONS
In this cohort of well-characterised patients with lean NAFLD without visceral adiposity, 33% (2/6) had rare monogenic drivers of disease, highlighting the importance of genomic analysis in this NAFLD subtype.
IMPACT AND IMPLICATIONS
Although most people with non-alcoholic fatty liver disease (NAFLD) are overweight or obese, a subset are lean and may have unique genetic mutations that cause their fatty liver disease. We show that 33% of study participants with NAFLD who were lean harboured unique mutations that cause their fatty liver, and that these mutations had effects beyond the liver. This study demonstrates the value of genetic assessment of NAFLD in lean individuals to identify distinct subtypes of disease.
背景与目的
非酒精性脂肪性肝病(NAFLD)的瘦型患者占受影响人群的10%-20%,其疾病驱动因素可能具有异质性。我们最近提议对无内脏肥胖的瘦型NAFLD患者进行评估,以寻找罕见的单基因疾病驱动因素。在此,我们旨在通过全外显子组测序,在一组经活检证实为NAFLD的特征明确的患者队列中验证这一框架。
方法
这项前瞻性研究纳入了124例经活检证实为NAFLD且有配对肝脏活检样本的患者,他们接受了标准化的研究访视,包括肝脏脂肪和硬度的高级磁共振成像(MRI)评估。
结果
识别出6例瘦型NAFLD患者并对其进行全外显子组测序。两名瘦型患者(33%)被确定患有单基因疾病。患有单基因疾病的瘦型患者与无单基因疾病的瘦型患者在年龄、人体测量学和MRI特征方面相似。患者1在醛缩酶B(ALDOB)中存在罕见的纯合致病突变,被诊断为遗传性果糖不耐受。患者2在载脂蛋白B(APOB)中存在罕见的杂合突变。该APOB变体(p.Val1856CysfsTer2)的致病性在英国生物银行中得到进一步验证,并与较低的循环APOB水平相关(β=-0.51g/L,95%CI -0.65至-0.36g/L,P=1.4×10⁻¹⁴)以及MRI上较高的肝脏脂肪相关(β=+10.4%,95%CI 4.3-16.5%,P=8.8×10⁻⁴)。因此,患者2被诊断为杂合性家族性低β脂蛋白血症。
结论
在这组特征明确的无内脏肥胖的瘦型NAFLD患者队列中,33%(2/6)有罕见的单基因疾病驱动因素,突出了基因组分析在这种NAFLD亚型中的重要性。
影响与启示
尽管大多数非酒精性脂肪性肝病(NAFLD)患者超重或肥胖,但有一部分是瘦型的,可能具有导致其脂肪性肝病的独特基因突变。我们表明,33%的瘦型NAFLD研究参与者携带导致其脂肪肝的独特突变,并且这些突变的影响超出肝脏。这项研究证明了对瘦型个体的NAFLD进行基因评估以识别不同疾病亚型的价值。
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