Late-onset stiff-person syndrome: challenges in diagnosis and management.

IF 4.7 2区 医学 Q1 CLINICAL NEUROLOGY Therapeutic Advances in Neurological Disorders Pub Date : 2023-12-25 eCollection Date: 2023-01-01 DOI:10.1177/17562864231214315
Marinos C Dalakas, Jessica Yi
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Abstract

Background: Stiff person syndrome (SPS) is a rare slowly progressive autoimmune neuronal hyperexcitability disease with very-high GAD-65 antibody titers that most commonly presents above the age of 20, with muscle stiffness, painful muscle spasms, slow gait, and falls leading to disability. In other autoimmune disorders, late-onset disease has different symptom-spectrum and outcomes, but there is no information regarding late-onset SPS (LOSPS).

Objective: Highlight delayed diagnosis and poor tolerance or incomplete response to therapies of patients with LOSPS and outline how best to increase disease awareness early at onset.

Design a retrospective chart reviewmethods: We reviewed GAD-positive SPS patients with symptom onset above age 60, identified among 54 SPS patients, examined, treated and followed-up by the same clinicians, focused on clinical presentation, misdiagnoses, response and tolerance to therapies, and evolved disability.

Results: Nine patients had LOSPS with symptom onset at median age of 61 years (range 60-78), and current median age of 73. The median time from symptom onset to SPS diagnosis was 3 years; prior to diagnosis, five patients were treated for lumbosacral radiculopathies (one with laminectomy), two for Parkinson's disease, one for multiple sclerosis, and another for cerebellar degeneration. Progressive decline occurred rapidly in all patients; at time of diagnosis, six patients were already using a cane or walker and two were wheelchair-bound. Tolerance and response to treatment were limited; two patients did not respond to IVIg, two discontinued IVIg despite early response due to comorbidities (cardiac disease, thrombosis), four others partially responded to IVIg and one to rituximab; several could not tolerate high doses of oral antispasmodics due to somnolence; and two patients died.

Conclusions: LOSPS is almost always misdiagnosed for other similar conditions commonly seen in the elderly. Patients with LOSPS decline quickly to clinically severe disease due to delayed treatment initiation, poor response or tolerance, other comorbidities, and possibly immunosenescence. Increased awareness that SPS can occur in the elderly mimicking other disorders is important for early diagnosis and treatment, even necessitating earlier immunotherapy initiation, compared to their younger counterparts, to prevent faster-evolving severe disability.

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晚发僵人综合征:诊断和管理方面的挑战。
背景:僵人综合征(SPS)是一种罕见的缓慢进展性自身免疫性神经元过度兴奋疾病,GAD-65抗体滴度非常高,最常见于20岁以上,表现为肌肉僵硬、肌肉痉挛疼痛、步态缓慢、跌倒导致残疾。在其他自身免疫性疾病中,晚发型疾病具有不同的症状谱和预后,但目前还没有关于晚发型 SPS(LOSPS)的信息。目的:强调晚发型 SPS 患者的诊断延迟、耐受性差或对治疗反应不完全,并概述如何在发病早期提高对疾病的认识:我们回顾了54名SPS患者中发病年龄在60岁以上的GAD阳性SPS患者,由相同的临床医生进行检查、治疗和随访,重点关注临床表现、误诊、对疗法的反应和耐受性以及逐渐发展的残疾:九名患者患有 LOSPS,发病年龄中位数为 61 岁(60-78 岁不等),目前年龄中位数为 73 岁。从症状出现到确诊为 SPS 的中位时间为 3 年;确诊前,5 名患者接受过腰骶部神经根病治疗(其中 1 人接受了椎板切除术),2 人接受过帕金森病治疗,1 人接受过多发性硬化治疗,还有 1 人接受过小脑变性治疗。所有患者的病情都在迅速恶化;确诊时,六名患者已经需要使用拐杖或助行器,两名患者需要坐轮椅。患者对治疗的耐受性和反应有限;两名患者对IVIg无反应,两名患者因合并症(心脏病、血栓)而在早期出现反应后停用了IVIg,另外四名患者对IVIg有部分反应,一名患者对利妥昔单抗有反应;几名患者因嗜睡而无法耐受大剂量口服解痉剂;两名患者死亡:结论:LOSPS几乎总是被误诊为其他常见于老年人的类似疾病。由于延迟开始治疗、反应差或耐受性差、其他并发症以及可能的免疫衰老,LOSPS 患者的病情很快恶化为临床重症。提高对 SPS 可模拟其他疾病发生在老年人身上的认识,对于早期诊断和治疗非常重要,甚至有必要比年轻人更早开始免疫治疗,以防止严重残疾的快速发展。
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来源期刊
CiteScore
8.30
自引率
1.70%
发文量
62
审稿时长
15 weeks
期刊介绍: Therapeutic Advances in Neurological Disorders is a peer-reviewed, open access journal delivering the highest quality articles, reviews, and scholarly comment on pioneering efforts and innovative studies across all areas of neurology. The journal has a strong clinical and pharmacological focus and is aimed at clinicians and researchers in neurology, providing a forum in print and online for publishing the highest quality articles in this area.
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