A Rare Case of Neuronal Ceroid Lipofuscinosis-Type 1 (NCL-1) with Vitamin D-Dependent Rickets-Type 1 (VDDR-1), Complex 1 Mitochondrial Deficiency, and Mixed Variant-Checkerboard and Phylloid Type of Pigmentary Mosaicism.

IF 0.4 Q4 PEDIATRICS
Journal of pediatric genetics Pub Date : 2024-05-30 eCollection Date: 2024-12-01 DOI:10.1055/s-0044-1787196
Vykuntaraju K Gowda, Anusha Raj K, Varunvenkat M Srinivasan, Dhananjaya K Vamyanmane, Sahana M Srinivas, Yasha Chickabasaviah, Rashmi Santhoshkumar, Pallavi Mittal, Surendra K Chikara, Gurudatta Baraka Vishwanathan
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引用次数: 0

Abstract

Introduction  Neuronal ceroid lipofuscinosis-type 1 (NCL-1) is a neurodegenerative lysosomal storage disorder. Vitamin D-dependent rickets type 1 (VDDR-1) is a rare cause of refractory rickets. Here, we report an unusual association of NCL-1 with VDDR-1. Case  A 3-year-old boy presented with a history of seizures from 45 days of life, delayed development, and loss of attained milestones at 20 months of age, along with progressive vision impairment since 1 year. Examination showed a failure to thrive, microcephaly, rachitic rosary, checkerboard and phylloid type of pigmentary mosaicism, fundus showed disc pallor with generalized narrowing of arterioles, bilateral retinitis pigmentosa, spasticity and dystonia, brisk reflexes, extensor plantar, and left choreoathetoid movements. Investigations showed hypocalcemia (7.8 mg/dL), normal phosphorus (3.9 mg/dL), elevated alkaline phosphatase (508.8 U/L), elevated parathyroid hormone (513.35 pg/mL), low 1,25-dihydroxy-vitamin D (9.93 pg/mL), and normal renal function. The child had metabolic acidosis, elevated ammonia (403.9 micromol/L), lactate (95 mg/dL, normal range 4.5-19.8 mg/dL), and creatine phosphokinase (432 U/L) level, and normal tandem mass spectroscopy. X-ray wrist showed healing vitamin deficiency rickets. Abnormal electroencephalogram was suggestive of low voltage activity. Magnetic resonance imaging brain showed gross cerebral and cerebellar atrophy. A muscle biopsy showed scattered atrophic fibers and several ultrastructural granular osmiophilic deposits and some mitochondrial aggregates of varying size were observed. Mitochondrial respiratory chain enzyme assay exhibited complex-1 deficiency (activity < 30%). Genetic analysis showed two pathogenic mutations: homozygous nonsynonymous variation c.674T > C in exon 7 of the PPT1 gene and a homozygous frameshift variation c.1178_1179delAA in exon 7 of CYP27B1 confirming the diagnosis of NCL-1 with VDDR-1. The child was treated with a low protein diet, levetiracetam, clonazepam, trihexyphenidyl, haloperidol, calcium supplement, calcitriol, and sodium benzoate; some improvement in clinical and biochemical parameters was noted on follow-up. Conclusion  This is a novel association of NCL-1 with VDDR-1 associated with complex-1 mitochondrial deficiency which has previously not been reported in the literature.

一例罕见的神经细胞类色素沉着病-1 型(NCL-1)伴维生素 D 依赖性佝偻病-1 型(VDDR-1)、线粒体复合体 1 缺乏症以及混合型变异-棋盘格和绒毛状色素镶嵌症。
导言 神经细胞类脂质沉着病 1 型(NCL-1)是一种神经退行性溶酶体储积症。维生素D依赖性佝偻病1型(VDDR-1)是一种罕见的难治性佝偻病。在此,我们报告了 NCL-1 与 VDDR-1 的不寻常关联。病例 一名 3 岁男童自出生 45 天起出现癫痫发作,发育迟缓,20 个月大时丧失里程碑,1 岁后出现进行性视力障碍。检查结果显示:发育不良、小头畸形、玫瑰疹、棋盘格和绒毛状色素镶嵌,眼底显示椎间盘苍白,动脉血管普遍狭窄,双侧视网膜色素变性,痉挛和肌张力障碍,反射亢进,足底外展,左侧舞蹈动作。检查结果显示:低钙血症(7.8 mg/dL),磷正常(3.9 mg/dL),碱性磷酸酶升高(508.8 U/L),甲状旁腺激素升高(513.35 pg/mL),1,25-二羟维生素D偏低(9.93 pg/mL),肾功能正常。患儿患有代谢性酸中毒,氨(403.9 微摩尔/升)、乳酸(95 毫克/分升,正常范围为 4.5-19.8 毫克/分升)和肌酸磷酸激酶(432 U/L)水平升高,串联质谱检查正常。腕部 X 光检查显示维生素缺乏性佝偻病愈合。异常脑电图提示低电压活动。脑部磁共振成像显示大脑萎缩和小脑萎缩。肌肉活检显示有散在的萎缩纤维,在超微结构上观察到一些颗粒状嗜锇沉积物和大小不等的线粒体聚集。线粒体呼吸链酶测定显示,PPT1 基因第 7 外显子中的复合体-1 缺乏(活性 C),CYP27B1 基因第 7 外显子中的同卵框移变异 c.1178_1179delAA 证实了 NCL-1 并发 VDDR-1 的诊断。患儿接受了低蛋白饮食、左乙拉西坦、氯硝西泮、三羟苯丙胺、氟哌啶醇、钙补充剂、钙三醇和苯甲酸钠等治疗,随访发现临床和生化指标有所改善。结论 NCL-1 与 VDDR-1 与复合体-1 线粒体缺乏有关,这是一种新的关联,以前从未在文献中报道过。
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来源期刊
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期刊介绍: The Journal of Pediatric Genetics is an English multidisciplinary peer-reviewed international journal publishing articles on all aspects of genetics in childhood and of the genetics of experimental models. These topics include clinical genetics, molecular genetics, biochemical genetics, medical genetics, dysmorphology, teratology, genetic counselling, genetic engineering, formal genetics, neuropsychiatric genetics, behavioral genetics, community genetics, cytogenetics, hereditary or syndromic cancer genetics, genetic mapping, reproductive genetics, fetal pathology and prenatal diagnosis, multiple congenital anomaly syndromes, and molecular embryology of birth defects. Journal of Pediatric Genetics provides an in-depth update on new subjects and current comprehensive coverage of the latest techniques used in the diagnosis of childhood genetics. Journal of Pediatric Genetics encourages submissions from all authors throughout the world. The following articles will be considered for publication: editorials, original and review articles, short report, rapid communications, case reports, letters to the editor, and book reviews. The aim of the journal is to share and disseminate knowledge between all disciplines in the field of pediatric genetics. This journal is a publication of the World Pediatric Society: http://www.worldpediatricsociety.org/ The Journal of Pediatric Genetics is available in print and online. Articles published ahead of print are available via the eFirst service on the Thieme E-Journals platform.
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