Landau Yuval E, Heimer Gali, Barel Ortal, Shalva Nechama, Marek-Yagel Dina, Veber Alvit, Javasky Elisheva, Shilon Aya, Nissenkorn Andreea, Ben-Zeev Bruria, Anikster Yair
Metabolic Disease Unit, Edmond and Lily Safra Children's hospital, Sheba Medical Center, Sackler Faculty of Medicine, Tel Aviv University, Israel.
Metabolic Disease Unit, Schneider Children's Medical Center, Sackler Faculty of Medicine, Tel Aviv University, Israel.
Mol Genet Metab Rep. 2020 Aug 15;25:100631. doi: 10.1016/j.ymgmr.2020.100631. eCollection 2020 Dec.
Peroxisomal D-bifunctional protein (DBP) deficiency is an autosomal recessive disorder historically described as a Zellweger-like syndrome comprising neonatal seizures, retinopathy, hearing loss, dysmorphic features, and other complications. The gene encodes DBP which is essential for oxidation of peroxisomal substrates. We describe 4 patients - 2 unrelated female girls and 2 monozygotic twin sisters - with DBP deficiency and phenotypic diversity.
Patient 1 presented neonatally with hypotonia and seizures, and later on developed global developmental delay and regression, sensorineural hearing loss, nystagmus and cortical blindness. The brain MRI demonstrated bilateral peri-sylvian polymicrogyria. Whole exome sequencing revealed 2 mutations in the gene (c.752G>A, p.(Arg251Gln); c.868 + 1delG).Patient 2 presented with hypotonia, motor delay, and sensorineural hearing loss in infancy, considerable developmental regression during her fourth year, nystagmus, and peripheral neuropathy. Brain MRI demonstrated cerebellar atrophy and abnormal basal ganglia and white matter signal, which appeared after the age of two years. Whole exome sequencing revealed 2 mutations in the gene (c.14 T>G, p.(Leu5Arg); c.752G>A, p.(Arg251Gln)).Patients 3 and 4, two female monozygotic twins, presented with hypotonia, developmental delay, and macrocephaly from birth, and later on also sensorineural hearing loss, infantile spasms and hypsarrhythmia, and adrenal insufficiency. Brain MRI demonstrated delayed myelination, and an assay of peroxisomal beta oxidation suggested DBP deficiency. Sequencing of the gene revealed the same 2 mutations as in patient 1.
We describe 4 patients with variable and diverse clinical picture of DBP deficiency and particularly emphasize the clinical, biochemical, and neuroimaging characteristics. Interestingly, the clinical phenotype varied even between patients with the exact two mutations in the gene. In addition, in two of the three patients in whom levels of VLCFA including phytanic acid were measured, the levels were within normal limits. This is expanding further the clinical spectrum of this disorder, which should be considered in the differential diagnosis of every patient with hypotonia and developmental delay especially if accompanied by polymicrogyria, seizures, sensorineural hearing loss, or adrenal insufficiency regardless of their VLCFA profile.
过氧化物酶体D-双功能蛋白(DBP)缺乏症是一种常染色体隐性疾病,以往被描述为一种类似泽尔韦格综合征,包括新生儿惊厥、视网膜病变、听力丧失、畸形特征及其他并发症。该基因编码对过氧化物酶体底物氧化至关重要的DBP。我们描述了4例DBP缺乏症且具有表型多样性的患者,其中2例为无血缘关系的女性患儿,2例为单卵双胞胎姐妹。
患者1出生时表现为肌张力减退和惊厥,随后出现全面发育迟缓及倒退、感音神经性听力丧失、眼球震颤和皮质盲。脑部磁共振成像(MRI)显示双侧外侧裂周围多小脑回。全外显子组测序揭示该基因存在2个突变(c.752G>A,p.(Arg251Gln);c.868+1delG)。患者2婴儿期表现为肌张力减退、运动发育迟缓及感音神经性听力丧失,4岁时出现明显发育倒退、眼球震颤和周围神经病变。脑部MRI显示小脑萎缩以及基底节和白质信号异常,这些在2岁后出现。全外显子组测序揭示该基因存在2个突变(c.14T>G,p.(Leu5Arg);c.752G>A,p.(Arg251Gln))。患者3和4为单卵双胞胎姐妹,出生时表现为肌张力减退、发育迟缓及巨头畸形,随后还出现感音神经性听力丧失、婴儿痉挛和高峰节律紊乱以及肾上腺功能不全。脑部MRI显示髓鞘形成延迟,过氧化物酶体β氧化检测提示DBP缺乏。该基因测序显示与患者1相同的2个突变。
我们描述了4例具有不同临床表现的DBP缺乏症患者,并特别强调了其临床、生化及神经影像学特征。有趣的是,即使是该基因存在完全相同的2个突变的患者,其临床表型也有所不同。此外,在3例检测了包括植烷酸在内的极长链脂肪酸(VLCFA)水平的患者中,有2例的水平在正常范围内。这进一步拓宽了该疾病的临床谱,对于每例肌张力减退和发育迟缓的患者,尤其是伴有多小脑回、惊厥、感音神经性听力丧失或肾上腺功能不全的患者,无论其VLCFA情况如何,在鉴别诊断时都应考虑到该病。
