Transient response to high-dose niacin therapy in a patient with NAXE deficiency

IF 1.8 Q2 Biochemistry, Genetics and Molecular Biology
JIMD reports Pub Date : 2024-05-09 DOI:10.1002/jmd2.12425
Fatema Al-Amrani, Khalid Al-Thihli, Eiman Al-Ajmi, Amna Al-Futaisi, Fathiya Al-Murshedi
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引用次数: 0

Abstract

Background

NAXE-encephalopathy or early-onset progressive encephalopathy with brain edema and/or leukoencephalopathy-1 (PEBEL-1) and NAXD-encephalopathy (PEBEL-2) have been described recently as mitochondrial disorders causing psychomotor regression, hypotonia, ataxia, quadriparesis, ophthalmoparesis, respiratory insufficiency, encephalopathy, and seizures with the onset being usually within the first three years of life. It usually leads to rapid disease progression and death in early childhood. Anecdotal reports suggest that niacin, through its role in nicotinamide adenine dinucleotinde (NAD) de novo synthesis, corrects biochemical derangement, and slows down disease progression. Reports so far have supported this observation.

Methods

We describe a patient with a confirmed PEBEL-1 diagnosis and report his clinical response to niacin therapy. Moreover, we systematically searched the literature for PEBEL-1 and PEBEL-2 patients treated with niacin and details about response to treatment and clinical data were reviewed. Furthermore, we are describing off-label use of a COX2 inhibitor to treat niacin-related urticaria in NAXE-encephalopathy.

Results

So far, seven patients with PEBEL-1 and PEBEL-2 treated with niacin were reported, and all patients showed a good response for therapy or stabilization of symptoms. We report a patient exhibiting PEBEL-1 with an unfavorable outcome despite showing initial stabilization and receiving the highest dose of niacin reported to date. Niacin therapy failed to halt disease progression or attain stabilization of the disease in this patient.

Conclusion

Despite previous positive results for niacin supplementation in patients with PEBEL-1 and PEBEL-2, this is the first report of a patient with PEBEL-1 who deteriorated to fatal outcome despite being started on the highest dose of niacin therapy reported to date.

Abstract Image

一名 NAXE 缺乏症患者对大剂量烟酸治疗的短暂反应
NAXE 脑病或早发性进行性脑病伴脑水肿和/或白质脑病-1(PEBEL-1)和 NAXD 脑病(PEBEL-2)最近被描述为线粒体疾病,可导致精神运动退化、肌张力低下、共济失调、四肢瘫痪、眼肌麻痹、呼吸功能不全、脑病和癫痫发作,通常在出生后三年内发病。它通常会导致疾病迅速发展,并在幼儿期死亡。轶事报道表明,烟酸通过其在烟酰胺腺嘌呤二核苷酸(NAD)从头合成中的作用,纠正了生化失调,并减缓了疾病的进展。我们描述了一名确诊为 PEBEL-1 的患者,并报告了他对烟酸治疗的临床反应。此外,我们还系统检索了接受烟酸治疗的 PEBEL-1 和 PEBEL-2 患者的文献,并审查了有关治疗反应和临床数据的详细信息。此外,我们还介绍了在标签外使用COX2抑制剂治疗NAXE脑病中与烟酸相关的荨麻疹的情况。迄今为止,已有7例PEBEL-1和PEBEL-2患者接受烟酸治疗的报道,所有患者对治疗均有良好反应或症状稳定。我们报告了一名PEBEL-1患者,尽管他的病情初步稳定,并接受了迄今为止报告的最高剂量的烟酸治疗,但结果却不容乐观。尽管之前对 PEBEL-1 和 PEBEL-2 患者补充烟酸取得了积极的效果,但这是首例 PEBEL-1 患者在开始接受最高剂量烟酸治疗后病情恶化并最终死亡的报告。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
JIMD reports
JIMD reports Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (miscellaneous)
CiteScore
3.30
自引率
0.00%
发文量
84
审稿时长
12 weeks
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