核上性麻痹是成年尼曼镰刀型 C 最初的表现形式

IF 3.2 Q2 CLINICAL NEUROLOGY Neurology International Pub Date : 2024-05-13 DOI:10.3390/neurolint16030042
Ali A. Mohamed, Willy Gan, Denis Babici, Veronica Hagan, Raphael Wald, Marc Swerdloff
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Herein, we present a rare case of NP-C1, diagnosed at age 35 with an initial symptom of supranuclear palsy. The goal of the presented case is to highlight the importance of the neurological examination and an inclusive differential diagnosis in patients with new-onset supranuclear palsy. (2) Methods: A single case report. (3) Results: A 46-year-old male with a past medical history of NP-C1 was admitted to the hospital for respiratory distress. He was noted to have a supranuclear gaze palsy with partially preserved voluntary saccades to the right. His mother revealed that he first had difficulty moving his eyes at the age of 34. After multiple consultations and genetic testing one year later, he was diagnosed with NP-C1. (4) Conclusions: Because NP-C1 affects many regions of the brain responsible for eye movements, neurological eye assessments can be a useful tool in diagnoses. 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引用次数: 0

摘要

(1) 背景:尼曼-皮克 C1 型(NP-C1)是一种溶酶体贮积症,会导致胆固醇和其他细胞脂质在内体-溶酶体途径中的转运缺陷。这种罕见的常染色体隐性遗传疾病根据发病年龄有三种表现形式。成人型患者的发病年龄超过 15 岁,但在 30 岁以后就很少见了。晚期成人型 NP-C1 的常见症状包括进行性认知障碍和共济失调,而精神病和运动障碍的发病率低于其他类型的 NP-C1。肌张力障碍性运动障碍最常见,此外还有舞蹈症、肌阵挛和帕金森病。在此,我们将介绍一例罕见的 NP-C1 病例,该患者在 35 岁时被确诊,最初的症状是核上麻痹。本病例旨在强调神经系统检查的重要性,以及对新发核上麻痹患者进行全面鉴别诊断的重要性。(2) 方法:单个病例报告。(3)结果:一名既往病史为 NP-C1 的 46 岁男性因呼吸困难入院。他被发现患有核上性凝视麻痹,部分自主向右侧眼球凝视功能保留。他的母亲透露,他在 34 岁时首次出现眼球移动困难。一年后,经过多次会诊和基因检测,他被确诊为 NP-C1。(4) 结论:由于 NP-C1 会影响大脑中负责眼球运动的多个区域,因此神经系统眼部评估可作为诊断的有用工具。此外,眼球运动异常可能是 NP-C1 最初出现的症状,容易使患者被误诊为进行性核上麻痹和其他可能与早期 NP-C1 相似的疾病。确诊需要通过基因检测。菲力平染色检测是过去的金标准。NP-C怀疑指数是为协助诊断而开发的,但其对晚期成人型NP-C1的疗效尚不明确。虽然目前尚无根治的方法,但早期识别有助于改善患者的症状管理过程。米格鲁司他是一种葡萄糖醛酸酰胺合成酶(GCS)抑制剂,是欧洲批准的专门针对 NP-C1 的疗法,用于减缓和预防 NP-C1 的神经系统表现。症状出现与开始治疗之间的延迟可能会导致较差的疗效和神经症状的恶化。大剂量可能会引起耐受性问题,尤其是在治疗延迟和神经功能缺损晚期的情况下。
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Supranuclear Palsy as an Initial Presentation of the Adult-Onset Niemann-Pick Type C
(1) Background: Niemann–Pick type C1 (NP-C1) is a lysosomal storage disorder that results in the defective trafficking of cholesterol and other cellular lipids in the endosomal–lysosomal pathway. This rare autosomal recessive disorder presents in three forms based on the age of onset. The adult form presents in patients greater than 15 years of age but is rarely seen after the age of 30. Common symptoms of the late adult-onset category of NP-C1 include progressive cognitive impairment and ataxia, with psychiatric and movement disorders presenting less frequently than in other forms of NP-C1. Dystonic movement disorders present most frequently, along with chorea, myoclonus, and parkinsonism. Herein, we present a rare case of NP-C1, diagnosed at age 35 with an initial symptom of supranuclear palsy. The goal of the presented case is to highlight the importance of the neurological examination and an inclusive differential diagnosis in patients with new-onset supranuclear palsy. (2) Methods: A single case report. (3) Results: A 46-year-old male with a past medical history of NP-C1 was admitted to the hospital for respiratory distress. He was noted to have a supranuclear gaze palsy with partially preserved voluntary saccades to the right. His mother revealed that he first had difficulty moving his eyes at the age of 34. After multiple consultations and genetic testing one year later, he was diagnosed with NP-C1. (4) Conclusions: Because NP-C1 affects many regions of the brain responsible for eye movements, neurological eye assessments can be a useful tool in diagnoses. Furthermore, eye movement abnormalities may be the initial presenting symptom of NP-C1, predisposing patients to misdiagnosis with progressive supranuclear palsy and other conditions that may mimic early-stage NP-C1. Definitive diagnosis is achieved through genetic testing. Filipin staining test was the gold standard in the past. The NP-C Suspicion Index was developed to assist in diagnoses, but its efficacy is unclear with late adult-onset NP-C1. Although no cure exists, early identification can facilitate an improved symptom management course for patients. Miglustat, a glucosylceramide synthase (GCS) inhibitor, is the approved therapy in Europe specific to NP-C1 for slowing and preventing the neurological manifestations of NP-C1. Delays between symptom onset and treatment initiation are likely to result in poorer outcomes and a progression of neurological symptoms. High doses may present tolerance concerns, especially in cases of delayed treatment and advanced neurological deficit.
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来源期刊
Neurology International
Neurology International CLINICAL NEUROLOGY-
CiteScore
3.70
自引率
3.30%
发文量
69
审稿时长
11 weeks
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