经典霍奇金淋巴瘤定向治疗加重brat1相关脑白质营养不良

IF 1.1 4区医学 Q4 CLINICAL NEUROLOGY

Neurologist Pub Date : 2024-05-01 DOI:10.1097/NRL.0000000000000539

Sara J Hooshmand, Karan L Chohan, Aditya Raghunathan, Deborah L Renaud, Michael W Ruff

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引用次数: 0

摘要

brca1相关的共济失调毛细血管扩张突变激活因子-1 (BRAT1)负责细胞周期监测和线粒体功能。成人发病的brat1变异的含义以及由此产生的表型神经认知和影像学特征以前没有被描述过。病例报告:一名66岁男性，最近诊断为经典霍奇金淋巴瘤，因认知和运动能力下降，核磁共振成像(MRI)显示进行性脑白质改变而被转介神经肿瘤学。神经学检查显示全身无力，步态广泛，双侧足底伸肌反应。脑MRI显示脑室周围、深部和皮层下白质T2/FLAIR高信号，无增强。脑脊液研究无显著差异。GeneDX遗传白质营养不良面板传导显示致病变异(c.294dupA;p.l 999tfsx92)导致BRAT1蛋白的截断，以及一个不确定意义的变异(c.746A>G;p.E249G)。推定诊断为继发于BRAT1变异的晚发性脑白质病。为了对抗他的线粒体功能障碍，他开始服用线粒体鸡尾酒，包括B-100复合物和辅酶Q10。他开始以淋巴瘤为导向的联合化疗，治疗2个周期后功能急剧下降。与化疗前显像相比，重复正电子发射断层扫描/计算机断层扫描代谢显像在化疗3个周期后出现应答;然而，重复脑部MRI显示弥漫性白质高信号恶化和脑萎缩。结论:考虑到表型和临床发病的可变性，白质营养不良可能是一个诊断挑战。该病例表现为进行性brat1相关脑白质营养不良，化疗引起的中毒性脑白质病加重。在多重代谢损伤的背景下，线粒体能量缺乏可能是遗传性白质营养不良病例中观察到的进行性神经衰退的基础。

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BRAT1-Associated Leukodystrophy Exacerbated by Classic Hodgkin Lymphoma-Directed Therapy.

Introduction: BRCA1-associated ataxia-telangiectasia-mutated activator-1 (BRAT1) is responsible for cell cycle surveillance and mitochondrial function. The implications of adult-onset BRAT1-variant and the resulting phenotypic neurocognitive and imaging features have not been previously described.

Case report: A 66-year-old man with a recent diagnosis of classic Hodgkin lymphoma was referred to neuro-oncology for cognitive and motor decline, and progressive cerebral white matter changes noted on magnetic resonance imaging (MRI). A neurological examination revealed global weakness, broad-based gait, and bilateral extensor plantar responses. Brain MRI demonstrated periventricular, deep, and subcortical white matter T2/FLAIR hyperintensities without contrast enhancement. Cerebral spinal fluid studies were unremarkable. A GeneDX genetic leukodystrophy panel conduction revealed a pathogenic variant (c.294dupA; p.L99TfsX92) resulting in a truncated protein of BRAT1, along with a variant of uncertain significance (c.746A>G;p.E249G). A presumptive diagnosis of late-onset leukoencephalopathy secondary to the BRAT1 variant was made. In an attempt to combat his mitochondrial dysfunction, he was initiated on a mitochondrial cocktail, including B-100 complex and coenzyme Q10. He began lymphoma-directed combination chemotherapy and developed precipitous functional decline after 2 cycles of therapy. Compared with prechemotherapy imaging, repeat positron emission tomography/computed tomography metabolic imaging showed a response after 3 cycles of chemotherapy; however, repeat brain MRI showed worsening diffuse white matter hyperintensities and cerebral atrophy.

Conclusion: Given the variability in phenotypes and clinical onset, leukodystrophies can be a diagnostic challenge. This case demonstrated progressive BRAT1-associated leukodystrophy exacerbated by chemotherapy-induced toxic leukoencephalopathy. Mitochondrial energy deficiency in the context of multiple metabolic insults was likely underlying the progressive neurological decline observed in this case of genetic leukodystrophy.

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来源期刊

Neurologist 医学-临床神经学

CiteScore

1.90

自引率

0.00%

发文量

151

审稿时长

2 months

期刊介绍： The Neurologist publishes articles on topics of current interest to physicians treating patients with neurological diseases. The core of the journal is review articles focusing on clinically relevant issues. The journal also publishes case reports or case series which review the literature and put observations in perspective, as well as letters to the editor. Special features include the popular "10 Most Commonly Asked Questions" and the "Patient and Family Fact Sheet," a handy tear-out page that can be copied to hand out to patients and their caregivers.