Chen Xiaodong, Zhou Jing, Li Rui, Zhang Bingjun, Wang Yuge, Zhong Xiaonan, Shu Yaqing, Chang Yanyu, Qiu Wei
Department of Neurology, The Third Affiliated Hospital of Sun Yat-sen University, Guangzhou, China.
Department of Neurology, Foshan First People's Hospital, Foshan, China.
J Clin Neurol. 2022 Jul;18(4):453-462. doi: 10.3988/jcn.2022.18.4.453.
Patients presenting with clinical characteristics that are strongly suggestive of neuromyelitis optica spectrum disorders (NMOSD) have a high risk of developing definite NMOSD in the future. Little is known about the clinical course, treatment, and prognosis of these patients with likely NMOSD at disease onset.
This study prospectively recruited and visited 24 patients with the limited form of NMOSD (LF-NMOSD) at disease onset from November 2012 to June 2021. Their demographics, clinical course, longitudinal aquaporin-4 immunoglobulin G (AQP4-IgG) serology, MRI, therapeutic management, and outcome data were collected and analyzed.
The onset age of the cohort was 38.1±12.0 years (mean±standard deviation). The median disease duration was 73.5 months (interquartile range=44.3-117.0 months), and the follow-up period was 54.2±23.8 months. At the end of the last visit, the final diagnosis was categorized into AQP4-IgG-seronegative NMOSD (=16, 66.7%), AQP4-IgG-seropositive NMOSD (=7, 29.2%), or multiple sclerosis (=1, 4.2%). Seven of the 24 patients (29.2%) experienced conversion to AQP4-IgG seropositivity, and the interval from onset to this serological conversion was 37.9±21.9 months. Isolated/mixed area postrema syndrome (APS) was the predominant onset phenotype (37.5%). The patients with isolated/mixed APS onset showed a predilection for conversion to AQP4-IgG seropositivity. All patients experienced a multiphasic disease course, with immunosuppressive therapy reducing the incidence rates of clinical relapse and residual functional disability.
Definite NMOSD may be preceded by LF-NMOSD, particularly isolated/mixed APS. Intensive long-term follow-up and attack-prevention immunotherapeutic management is recommended in patients with LF-NMOSD.
具有强烈提示视神经脊髓炎谱系障碍(NMOSD)临床特征的患者,未来发展为确诊NMOSD的风险很高。对于这些疾病发作时可能患有NMOSD的患者的临床病程、治疗及预后知之甚少。
本研究前瞻性招募并随访了2012年11月至2021年6月疾病发作时的24例有限型NMOSD(LF-NMOSD)患者。收集并分析了他们的人口统计学资料、临床病程、纵向水通道蛋白4免疫球蛋白G(AQP4-IgG)血清学、MRI、治疗管理及结局数据。
该队列的发病年龄为38.1±12.0岁(均值±标准差)。疾病持续时间中位数为73.5个月(四分位间距=44.3-117.0个月),随访期为54.2±23.8个月。在最后一次随访结束时,最终诊断分为AQP4-IgG血清阴性NMOSD(=16,66.7%)、AQP4-IgG血清阳性NMOSD(=7,29.2%)或多发性硬化(=1,4.2%)。24例患者中有7例(29.2%)发生了向AQP4-IgG血清阳性的转化,从发病到这种血清学转化的间隔时间为37.9±21.9个月。孤立/混合性最后区综合征(APS)是主要的起病表型(37.5%)。孤立/混合性APS起病的患者更倾向于转化为AQP4-IgG血清阳性。所有患者均经历多相病程,免疫抑制治疗降低了临床复发率和残余功能残疾率。
确诊NMOSD之前可能先有LF-NMOSD,尤其是孤立/混合性APS。建议对LF-NMOSD患者进行长期密切随访及预防发作的免疫治疗管理。
